Cell atlas of the healthy and ulcerative colitis human colon

ABSTRACT

The present invention provides for a human cell atlas of the colon from healthy and diseased subjects. The atlas was obtained by single sequencing of about 117,000 cells. The present invention discloses novel markers for cell types. Moreover, genes associated with disease are identified in the colon and colon specific cell types. The invention provides for diagnostic assays based on gene markers and cell composition, as well as target cell types that express genes associated with disease. Finally, disclosed are novel cell types and methods of quantitating, detecting and isolating the cell types.

CROSS-REFERENCE TO RELATED APPLICATIONS

This application claims the benefit of U.S. Provisional Application Nos. 62/533,638, filed Jul. 17, 2017, 62/581,424, filed Nov. 3, 2017 and 62/692,541, filed Jun. 29, 2018. The entire contents of the above-identified applications are hereby fully incorporated herein by reference.

STATEMENT REGARDING FEDERALLY SPONSORED RESEARCH

This invention was made with government support under Grant Nos. OD020839, AI089992, CA217377, AI039671, AI1118672, HG006193 and CA202820 awarded by the National Institutes of Health. The government has certain rights in the invention.

REFERENCE TO AN ELECTRONIC SEQUENCE LISTING

The contents of the electronic sequence listing (“BROD-2203US_ST25.txt”; Size is 4,929 bytes and it was created on Nov. 23, 2020) is herein incorporated by reference in its entirety.

TECHNICAL FIELD

The subject matter disclosed herein is generally directed to a cell atlas of the human colon in healthy and disease states. The subject matter further relates to novel cell specific and disease specific markers.

BACKGROUND

Tissues function through the coordinated actions of diverse parenchymal, immune, and stromal cell types responding to local and distal cues. Breakdown in any cellular compartment can lead to disease, due to intrinsic cell dysfunction or through compensations by other cells to restore tissue homeostasis. This intricate interplay among cells makes it difficult to determine the causal cellular mechanisms that initiate or promote disease. In the past, measuring the contribution of each cellular compartment was hampered by the need to average bulk measurements across the entire tissue or to assess known cell subsets or selected genes a priori.

The small intestinal mucosa is a complex system. The mucosa comprises multiple cell types involved in absorption, defense, secretion and more. These cell types are rapidly renewed from intestinal stem cells. The types of cells, their differentiation, and signals controlling differentiation and activation are poorly understood. The small intestinal mucosa also possesses a large and active immune system, poised to detect antigens and bacteria at the mucosal surface and to drive appropriate responses of tolerance or an active immune response. Finally, there is complex luminal milieu which comprises a combination of diverse microbial species and their products as well as derivative products of the diet. It is increasingly clear that a functional balance between the epithelium and the constituents within the lumen plays a central role in both maintaining the normal mucosa and the pathophysiology of many gastrointestinal disorders. Many disorders, such as irritable bowel disease, Crohn's disease, and food allergies, have proven difficult to treat. Inflammatory bowel disease (IBD) is a group of inflammatory conditions of the colon and small intestine, principally including Crohn's disease and ulcerative colitis, with other forms of IBD representing far fewer cases (e.g., collagenous colitis, lymphocytic colitis, diversion colitis, Behçet's disease and indeterminate colitis). Pathologically, Crohn's disease affects the full thickness of the bowel wall (e.g., transmural lesions) and can affect any part of the gastrointestinal tract, while ulcerative colitis is restricted to the mucosa (epithelial lining) of the colon and rectum. Some of the genetic factors predisposing one to IBD are known, as explored in Daniel B. Graham and Ramnik J. Xavier “From Genetics of Inflammatory Bowel Disease Towards Mechanistic Insights” Trends Immunol. 2013 August; 34(8): 371-378 (incorporated herein). The manner in which these multiple factors interact remains unclear.

A case in point is ulcerative colitis (UC), a major subtype of Inflammatory Bowel Disease (IBD), where inflammation begins in the rectum and extends proximally in a contiguous fashion. Left-sided disease is characterized by a sharp demarcation between inflamed and non-inflamed segments. Explaining the geographical restriction of UC remains a challenge. While endoscopic examination followed by histological analysis are the current standard of care, they fail to capture key aspects of the disease, including immune cell activation states, cell-specific cytokine profiles, and disease-related features of stromal cells, and do not distinguish the pathways associated with chronic inflammation from attempts at disease restitution. Furthermore, several genes mapped by genome-wide association studies (GWAS) as associated with disease risk suggests a critical role for the intestinal barrier in preventing IBD, with defects in autophagy, ER stress, oxidative stress, cell death, IL23R/Th17 biology, immune tolerance, solute transport and perturbed innate and adaptive immune signaling [REF]. However, the cellular compartments and cell-cell interactions in which these GWAS genes and pathways act are often unknown.

Single-cell RNA-Seq (scRNA-Seq) can help advance our understanding of complex disease by comprehensively mapping the cell types and states in the tissue, distinguishing changes in cell-intrinsic expression programs from cell-extrinsic changes in cell frequencies, and predicting how these connect through cell-cell interactions. When comparing healthy and disease tissue, this may help determine with precision: which cell populations are disrupted in disease? Which cell-intrinsic programs are changed? What cell-cell interactions affect cell recruitment during inflammation and disease resolution? What are the cells-of-action of disease risk genes? and, What are the effects of current therapies and how might therapeutic resistance arise? Unlike bulk profiling, which averages across cell types, scRNA-Seq can readily distinguish between cell-intrinsic changes in expression program and cell-extrinsic changes in cell frequencies and cell-cell interactions. Unlike most in situ methods, which require prior knowledge of the genes and proteins of interest, scRNA-Seq can in principle do so systematically across all cells and programs in the tissue ecosystem, including those that may not yet be known to present in the tissue. This approach has been demonstrated for tumors (see, e.g., Tirosh, et al., Dissecting the multicellular ecosystem of metastatic melanoma by single-cell RNA-seq. Science 2016, 352, 189-196), but not yet for other complex immune mediated diseases, such as UC, where the window for disease onset, activity and resolution is measurable with endoscopic biopsies.

For example, Inflammatory bowel disease (IBD) is a chronic and debilitating disorder that affects millions of people worldwide. IBD is heterogeneous, comprising two main subtypes, Crohn's disease (CD) and ulcerative colitis (UC), which have different risk factors and clinical presentations. CD patients typically have discontinuous inflammation that extends deep into the mucosa throughout the gastrointestinal tract, while UC patients have continuous inflammation that is largely restricted to the mucosa of the large intestine. IBD is thought to arise from a maladaptive immune response to the gut Here, Applicants used intestinal biopsies microbiota in a genetically susceptible host. Genome-wide association studies (GWAS) have pinpointed hundreds of IBD-associated loci that explain ˜10% of disease susceptibility. While linkage disequilibrium has precluded mapping most loci to single variants, fine-mapping studies have directly implicated several genes, including NOD2, IL23R, ATG16L1, and PTPN22. Functional analysis of these genes suggests a critical role for the intestinal barrier in preventing IBD, with defects in autophagy, immune signaling, and epithelial barrier function leading to elevated disease risk. However, the functional roles for most such genes are unknown and the ability of GWAS to detect causal variants exceeds our ability to generate functional insights into the disease.

SUMMARY

In certain example embodiments, the present invention provides for a human cell atlas of the colon for healthy and disease states and methods of use. This disclosure provides a rationale for modulating intestinal cell balance, function, differentiation and/or activity for the treatment of both IBD and other disorders.

In certain embodiments, the IBD is Crohn's disease or ulcerative colitis. In certain embodiments, the IBD is collagenous colitis, lymphocytic colitis, diversion colitis, Behçet's disease, or indeterminate colitis.

In one aspect, the present invention provides for a method of detecting inflammatory bowel disease (IBD) comprising measuring in a biological sample obtained from the gastrointestinal tract of a subject the frequency of one or more cell types selected from the group consisting of B cells, T cells, endothelial cells, epithelial cells, fibroblasts and myeloid cells compared to the total of all cell types in the sample, wherein IBD is detected when the frequency of one or more cell types is altered as compared to a healthy frequency. The one or more cell types may be selected from the group consisting of colitis-associated inflammatory fibroblasts (CAIFs), absorptive transit amplifying (TA) 1 cells, absorptive TA 2 cells, class switching B cells, crypt fibroblasts (loFos), glial cells, goblet 1 cells, neutrophils, plasma B cells, post-capillary venules and tolerogenic DCs.

In certain embodiments, the cell type may be detected by measuring one or markers for each cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12. The top 250 markers for each cell type are listed in ranked order.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in a biological sample obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide selected from the group consisting of: MTRNR2L1, HLA-B, CHI3L1, EIF5A, RPL3, S100P, TIMP1, REG1A, C8orf4, HMGCS2, DMBT1, AC005540.3, OLFM4, IL13RA2, MMP3, REG4, IGJ, DEFA5, TNFRSF12A, BGN, SELENBP1, TPM4, IFITM2, TNFRSF11B, PKM, PHLDA1, MT1G, LGALS4, IGFBP5, URAD, ANXA2, HLA-DRA, PLA2G2A, PDPN, S100A11, SELL, SOD2, LDHA, SMDT1, CCL8, FCGRT, RPL9, CYR61, NNMT, LMNA, HIF1A, CD82, LINC00152, TAGLN2, IFITM3, EMP1, AKR1C1, CD63, FKBPlA, PTMA, COL6A3, REG3A, BACE2, C10orf99, CNN3, CEBPB, RPL13A, LCN2, HSPA1B, CKB, PHGR1, CD59, Cllorf96, ANXA5, RPL18A, COL4A1, CTHRC1, PCOLCE, COL1A1, FTL, EMP3, GEM, COL4A2, PRSS23, S100A6, S100A3, CA1, REG1B, TNC, CCR7, MEOX1, FGF7, MMP1, RPS3A, THY1, RPS26, PKIB, CHP2, SERPINE1, TXNIP, COL6A1, RPS4Y1, PSME2, CAV1, ANGPTL2, TAGLN, TFF1, HGF, PDIA3, CDH13, ACADS, KDELR2, NOP10, SELM, HAPLN3, FABP4, PTGES, DSTN, CCL5, VAMP8, MT-ND1, SERPINHI, HYI, POLR2L, PPIB, HLA-DMA, TST, AQP1, SPARC, CA2, CCL13, MT-CYB, HLA-DPB1, SPINK1, AQP8, ATOX1, RPL37A, IER3, ENOl, MT1H, HSPA5, HSPA1A, ITM2C, SDC2, ID1, AMN, FABP6, PIGZ, COL8A1, DUOXA2, TPM2, CRIP2, HYAL2, CPXM1, NCOA7, RPS29, TMEM258, CLDN7, PHLDA2, TMSB10, F2R, PXMP2, SRM, CFB, NDUFA4L2, CBX3, NXPE4, ACAA2, NDRG2, KANSL1-AS1, KLF2, LAPTM4A, ITGA5, DHRS4, CDX2, PRKCDBP, RPL6, SOCS3, GPR160, PPDPF, SEPP1, TMEM141, ELP5, NRG1, SPON2, CXCL1, ID3, PTRF, CALR, TMEM165, HSP90B1, CLEC9A, INHBA, SPHK1, FABP1, LGALS2, PDLIM4, TMEM158, CKMT1A, TRMT112, CCDCl₃, HOXB13, MRGPRF, CALU, ACSF2, MMP10, VSIG2, RAMP1, MT1M, APOA4, TFPI2, FXYD3, MORF4L1, PEBP1, STAP2, NFKBIA, MT-C03, DHRS11, SPINT2, PRRX2, RCN3, EIF4A1, TUBB, TSHZ2, KRT8, ACTN1, VAMP5, RPL10, IL11, AGT, SERPINA1, SLC26A2, CLU, APOBEC3B, DNAJB1, THBS2, UBD, PIM3, PRKAR1A, IL32, IGFBP7, UGT2A3, HLA-DRB5, PPA1, CHCHD10, COL6A2, CD55, RNASET2, CTGF, MT-CO1, CTSK, C19orf10, SERPINE2, HSD17B12 and SAA1; or MTRNR2L1, HLA-B, RPL3, TIMP1, IGJ, IFITM2, CCR7, CCL5 and IGFBP7; or MTRNR2L1, HLA-B, RPL3, TIMP1, IGJ, IFITM2, CCR7, CCL5 and IGFBP7; or genes in Table 4, 6, 8, 13, 14 or 15, wherein the genes or polypeptides are differentially expressed in IBD as compared to a healthy gastrointestinal tract reference level. The expression of MTRNR2L1, HLA-B, TIMP1, CCR7, IFITM2, and IGFBP7 may be upregulated as compared to a healthy reference level and the expression of RPL3, IGJ and CCL5 may be downregulated as compared to a healthy reference level.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in B cells obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide specific for the indicated cell type in brackets selected from the group consisting of: [Plasma_B_cells] G0S2, FABP1, TNFRSF18, PHGR1, AGR2, GAS6, RPL3, LMNA, TIMP1, SMOC1, HIST1H1C, HSP90AA1, TNFRSF4, HSPA1A, HSPA1B, CYP20A1, KRT19, CXCR4, DNAJB1, XBP1, GOLGA2 and CADM1; or [Class_switching_B_cells] TIMP1, RPL3, HSP90AA1, LMNA, ILVBL, CD69, CTHRC1, TNFRSF4, G0S2, PABPC4, ITM2C, AGR2, RPS3A, RNASE6, LGALS4, HLA-DMA, FXYD3, PTMA, TNFRSF18, RP11-16E12.2, H3F3B, KLF6, QPRT, TPM4 and SMOC1; or [Follicular_B_cells] C12orf75, METAP2, CCND3, HLA-DQB1, HLA-DRB5, RPS4Y1, TUBB2A, LCK, RMI2, SMARCB1, HLA-DPB1, TCEA1, MME, RPL9, SLBP, CD63, UBE2D3, A4GALT, PLD4, SIT1, PPP1CC, PAIP2, CCDC109B, DCAF12, SRSF3, HLA-DQA1, HLA-C, ISG20, HMGN1, HMCES, HNRNPC, HLA-DPA1, TUBB2B, HNRNPA3, CD27, EIF1AY, ITGAE, TPD52, ECHS1, RAP1B, HLA-DQA2, GGA2, CHCHD10, ACTR3, HLA-DRA, SGPP1, PGAM1, DCK, TSG101, HNRNPM, LTB, CLIC4, LSM10, GDI2, RGS16, CAPG, SRSF2, ZFAND2A, RPL36, CBX3, AGR2, MRPL47, TRA2A, FBL, SELT, SUMO2, HADHB, DEF8, FGD2, LIMD2, PSIP1, RBBP7, BZW1, TSTD1, MTF2, IKZF1, RUVBL1, BACH2, PIM1, CHRAC1, EZR, MCM5, IGJ, COX6B1, PRPSAP2, TK1 and CCR7.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in endothelial cells obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide specific for the indicated cell type in brackets selected from the group consisting of: [Microvascular_cells] PLAT, AQP1, CD9, HLA-A, HLA-DRA, EGLN3, LDHB, HLA-C, RBP5, CD99, PASK, S100A10, SERPINE1, CXCL12, JUN, ANXA2, TESC, IGJ, FOSB, LIMS1, HSPA1A, CALU, RCN3, S100A6, CST3, PRSS23, SEPP1, HSPA1B, WWTR1, RAMP1, GPX4, PSMB9, PSME2, CTGF, CD82, LGALS4, SNED1, TNFRSF4, IER3, VAMP8, ALDOA, HLA-B, TAP1, CD36, F2RL3, KDR, COL15A1 and PLAU; or [Post-capillary_venules]PTGS1, RAMP1, PDLIM1, HLA-A, OLFML3, PLAT, STXBP6, UBD, LY6E, TNFSF10, CD9, MGP, CPE, PSMB8, PHLDA1, EIF4A2, GIMAP7, TMEM100, CST3, HLA-C, RPL9, RPL10, LPCAT4, AQP1, GIMAP1, SRPX, MALAT1, RPL3, AGR2, PRSS23, COL4A3BP, EFEMP1, SNHG7, TUBAIB, PTGES, NFKBIZ, B2M, FTH1, C19orf66, CDKN3, RNF181, EEF1B2, MDK, CLIC1, TPTEP1, TFF3, S100A10, JUN, CRIP1 and MED24; or [Vitamin metabolizing]PLAT, CXCL12, ENPP2, TXNIP, IGFBP4, CD36, ANXA2, OAZ2, CD320, AQP1, CTGF, RGS5, TGFBR2, RAMP1, CD9, C16orf80, CXCR4, CLDN5, STC1, GJA1, FAM213A, PLAU, HLA-E, PRKCDBP, RBP5, RPL9, SAT1, TNFSF10, S100A4, TSPAN7, AKR1C3, C8orf4, HLA-DPB1, SRP14, TNFRSF4, TIMP1, ANXA1, Clorf54, RND1, ANGPT2, EGR1, STAT3, SH3BP5, RPL29, CTNNBIP1, LSMD1, HLA-C, RBM17, GYPC, NDUFA7, IER2, COTL1, RPLPO, SDPR, IDIl, SLC6A6, RPL10A, MYL6, AQP3, NKX2-3, COASY and SOD2; or [Endothelial_pericytes] FAM222B, RP11-490M8.1, TWF2, ZNF205 and HYI.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in epithelial cells obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide specific for the indicated cell type in brackets selected from the group consisting of: [Enterocytes] SPINK1, PLA2G2A, IL18, ATP1B3, MTRNR2L1, GSTP1, GPX2, CYBA, TAX1BP3, S100A14, NQO1, TSPAN3, NAALADL1, CTSA, RARRES3, OAS1, LGALS1, HMGCS2, PCK1, PRDX5, MUC1, TMEM37, KRTCAP3, MT2A, MX1 and S100A11; or [Tuft cells] PTGS1, ESYT2, SHC1, HPGDS, HOOK1, BCKDK and RALGAPA1; or [Goblet 2] SPINK4, NUPR1, S100A14, BAIAP2L1, BDKRB1, MT-ND2, FAM3B, MUC13, TFF1, ANO9 and TUBB2A; or [Absorptive_TA_1] REG1A, CD74, RPL3, HLA-DRB1, MT2A, RPS3A, ARHGDIB, TIMP1, LIN7C, MTRNR2L1, KCNK6, RPL18A, TNFRSF12A and SEC1IC; or [Secretory_TA] HLA-DRA, HLA-DRB1, RARRES2, ID3, HLA-DMA, UGT2B17, CD74, HLA-DRB5, REG1A, HLA-DPB1, HLA-DPA1 and GLB1L2; or [Absorptive_TA_2] AGR2, HLA-DRA, CD74, S100A11, HSPB1, SPINK1, HLA-DRB1, TIMP1, RARRES3, SELENBP1, GPX2, MUC12, ID3, ARHGDIB, REG1A, PLA2G2A, CEACAM5, IDH2, IGJ, RNASET2, BSG, PSMB9, ADIRF, LEFTY1, RARRES1, LYZ, MTRNR2L1, TFF1, RPS4Y1, SRSF6, CNPY2, GSTP1 and ATP1B3; or [Cycling_TA] RARRES2, ARHGDIB, IGJ, BST2, PKIG, PITX1, ETS2, HLA-DRA, TIMP1, MTRNR2L1, HRCT1, ZNF90, MUC12, AKR1B1, HLA-DPA1, VAMP7, S100P, NQO1, DEK, ABRACL, REG1A, ACAT1, DNAJB1, HLA-DRB1 and IGFBP4; or [Goblet 1] SPINK4, ITLN1, IGJ, AGR2, SDF2L1, TIMP1, PDLIM1, MUC2, LYZ, SELK, HMGCS2, SEC11C, SSR4, DNAJA1, FKBP11, REG4, EZR, SELM, CISD1, SYTL1, PHLDA2 and CHPF.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in fibroblasts obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide specific for the indicated cell type in brackets selected from the group consisting of: [Inflammatory fibroblasts] COL1A2, GBP1, IFI27, DYNLT1, PKM, PHLDA1, DUSP1, CNOT4, CCL8, LAP3, ACP5, GSTT1, GALNT11, PSMB9, TNIP2, PSMB8, HAPLN3 and PERP; or [Fibroblast_pericytes] NET1; or [Myofibroblasts] PDLIM7, NBL1, C12orf75, PHLDA2, IGFBP5, PRSS23, TM4SF1, SQRDL, MRGPRF, RERG, MXRA8, RPS4Y1, EGR1, HOXD9, TDO2, DUSP1, LMNA, CYB5R3, DDAH2 and TFPI2; or [Villus_fibroblasts] MMP2, SRPX2, TNC, MMP1, S100A4, NSG1, EDNRB, AGT, TRPA1, CPE, VSTM2A, RBP4, TSHZ2, IL32, VASN, CRIP1, NR4A2, PCTP, PRSS23, MCL1, NDUFA4L2, ANXA1, TMSB4X, PDLIM1, IGFBP3, CEBPD, FOXF1, ACP1, CiS, FRZB, ECM1, DMKN, ID4, PDGFRA, GADD45B and SPARCL1; or [Crypt fibroblasts_(hiFos)] TM4SF1, VASN, GSN, FGF7, PLAT, CLEC14A, IQGAP2, ID3, FN1, SEPP1, TNXB, CCL13, TPBG, HSD17B2, STMN2, GPX3, VIM and TNFSF10; or [Crypt fibroblasts_(loFos)] GPX3, NR4A1, CiS, TM4SF1, DUSP1, ID1, LGALS3BP, COL15A1, SERPINGI, TNFAIP6, CFD, ADAMDEC1, MZT2B, MIF, EGR1, DKK3, NBEAL1, GSN, GGT5, FOXF1, RPL9 and CD74.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in macrophages obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide specific for the indicated cell type in brackets selected from the group consisting of LGMN, RNASE1, AKR1B1, LGALS2, A2M, C15orf48, VMO1, SERPINFI, SPINT1, ACP5, TFF3, RNASET2, ENPP2, LGALS1, MMP9, CORO1A, CSTB, SELK, MT2A, FBP1, PLSCR1, FXYD5, NR1H3, UCHL3, SEPP1 and AGR2.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in T cells obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide specific for the indicated cell type in brackets selected from the group consisting of: [T_cells] NUB1, CAV1, EIF2S1, COL6A1, POSTN, ALAS1 and RGCC; or [Activated_CD4_cells_loFos] S100A4, RPS29, TIMP1, RPL9, CFL1, VIM, ANXA1, PHLDA1, S100A11 and HLA-A; or [Activated_CD4_cells_hiFos] IGJ and ADSS; or [CD8_IELs] CCL3, CCL4, RPL10, RPL6, CD3E, MTRNR2L1, ARHGDIB, CD3G, RPL3, ITGB2, KLRB1, IFNG, RPL22, RPL18A and PTMA; or [CD8_LP_cells] RPL9, EMP3 and ARFRP1; or [Tregs] CD7, CD2, TIAl and GRSF1; or [Memory_T_cells] RPL9, PFN1, IL32, ANXA1, S100A4, ARPClB, KLRB1, RPL30, ANAPC5, GAPDH, B2M, RPS28, PSME2, AK5, SERF2, RILPL2, RPS29, TAGLN2, FXYD5, S100A11, ANXA5, S100A6, PNRC1, ARPC2 and ZFP36; or [Cycling_CD8_cells] ENTPD1, CD2, EIF5A, LCK, HAVCR2, ATP5L, KLRB1, CALR, MTPN, CENPA and MIF.

In another aspect, the present invention provides for a method of detecting IBD comprising measuring in cells obtained from the gastrointestinal tract of a subject the expression of a gene or polypeptide specific for the indicated cell type in brackets selected from the group consisting of: [Stem_cells] AQP1, RPL3, RPS4Y1, LYZ, LCN2, ID3, HLA-DRA, HLA-DRB1, HLA-DMA, HLA-DPA1, C2, NQO1, B2M, ARHGDIB, DNAJB1, RARRES2, MTRNR2L1, HLA-C, CD74, C19orf70, GSTT1, TESC, IFI27, PSME1, HMGCS2, HLA-DRB5, RPL6, UGT2B17, HLA-DPB1, PSMB9 and SCARB2; or [Enteroendocrine] RARRES2, HLA-DRA, SEC11C, MT2A, NIPSNAP1, OLFM4, DDC, MDK and CD82; or [Glial_cells] ALDH1A1, CLU, ANXA1, SPP1, IL32, CAPS, FIBIN, RPL3, RPL9, HLA-G, MRPS6, LINC00152, HOXC6, CDKN2A, TUBA1A, HLA-DQA2, SOCS3, SEPP1, IGJ, HLA-DRB5, KLC1, HLA-DRB1, NDUFB4, ENTPD2, SRGN, PMEPA1, HSPA1B, FKBPlA, GLIPR2, UBR4, UBB, COX7A1, LSM3, PRDX2 and NUPR1; or [Dendritic_cells] CST3, MARCKSL1, CD52, PPA1, IGJ, SERPINBI, TYMP, STMN1, FCER1A, DNAJB1 and PRELIDI; or [Mast cells], NFKBIZ, EGR3, IL1RL1, HLA-B, CAPG, EGR2, HLA-C, RPS4Y1, CTSW, EIF4G2 and ZEB2; or [Cycling_monocytes] TFF3, ATP2A3, GSDMD, EMP3, IL12RB1, PSMD11, ENPP2, ALOX5AP and AKl; or [Tolerogenic_DCs] TXN; or [Neutrophils] GBP1, FCGR2B, GSTO1, RPL30, TMEM176B, EMG1 and GDI2; or [NK_cells] ILF3, CALCOCO2 and CD47.

In certain embodiments, the cell type according to any embodiment herein may be obtained by sorting cells based on expression of one or markers for each cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12. The sorting may be performed by deconvolution of bulk expression data in silico. Not being bound by a theory, the quantity of cells may be determined by cell specific markers and gene expression assigned to each cell. The biological sample according to any embodiment herein may be obtained by colonoscopy.

In another aspect, the present invention provides for a method of treating IBD comprising modulating the activity of one or more gastrointestinal tract cell types selected from the group consisting plasma B cells, class switching B cells, follicular B cells, microvascular cells, post-capillary venules, vitamin metabolizing, endothelial pericytes, enterocytes, tuft cells, goblet 2, absorptive TA 1, secretory TA, absorptive TA 2, cycling TA, goblet 1, stem cells, enteroendocrine, glial cells, inflammatory fibroblasts, fibroblast pericytes, myofibroblasts, villus fibroblasts, crypt fibroblasts (hiFos), crypt fibroblasts (loFos), T cells, macrophages, dendritic cells, mast cells, cycling monocytes, tolerogenic DCs, neutrophils, activated CD4 cells loFos, activated CD4 cells hiFos, CD8 IELs, CD8 LP cells, Tregs, memory T cells, NK cells and cycling CD8 cells. The one or more cell types may express one or more IBD GWAS genes selected from the group consisting of: IL32, MHCII, RNF186 and SLC39A8; or LMAN2, ATF4, TRIB1, HSPA6, RABEP2, CAMP, TSPAN14, STRN4, MOB2, HYAL1, DOCK9, CTSA, TST, PLEKHG6, RHPN2, C2CD2L, D2HGDH, REG4, DDC, HCK, MED16, GRB7, SPRED2, COG5, ADK, RIT1, SLC15A3, PLAU, ING5, NF2, PDLIM7, ZP1, PLA2G4A, CCL13, TTYH3, NFKBIZ, VPS11, CARD9, TNNI2, RIPK2, GPBAR1, SLC11A1, IFNG, CD28, EIF3G, CUL1, FASLG, MXD3, TCF19, DPAGT1, PHTF1, HOXA5, COX15 and LIF; or [GPCR] CCR10, GPRC5D, GPR18, CXCR5, CALCRL, F2RL3, FZD4, SlPRl, GPR4, APLNR, FZD6, LPAR6, GPR146, AVPR2, HRH1, GPRC5B, TBXA2R, GPRC5A, FZD5, GPR39, LGR5, VIPR1, F2RL1, LGR4, OPN3, FFAR4, GPR153, GPR37L1, FZD3, LPAR1, GPR137, SMOX, ADORA2B, BDKRB1, PGF, ADRA2A, PTGIR, EDNRA, MRGPRF, F2R, EDNRB, GLP2R, PTGFR, ACKR3, FZD1, ADORA1, ADORA3, CMKLR1, FPR3, P2RY13, ADRB2, LPAR5, P2RY14, GPR34, PTAFR, CCRL2, GPBAR1, FFAR2, C5AR1, C3AR1, CCR1, FPR1, GPR82, CXCR6, CCR7, DHX15, CCR6, GPR68, PTGDR and LTB4R; or [cell-cell interaction] TNFRSF17, SEMA4A, EBI3, RAMP3, ROBO4, F2RL3, APLN, NRP2, CCL21, ICAM2, PLXND1, HRH1, EPHA2, CGN, CELA3B, CFTR, RGMB, SCT, AZGP1, TSPAN1, IL22RA1, IL1R2, RSPO3, NRXN1, NCAM1, ANGPTL2, TNC, MMP1, COL18A1, C1QTNF1, COL5A3, NEO1, NTN1, BMP2, TSLP, SEMA3A, PROS1, ANGPTL1, CCL19, CD4, LY96, IL5RA, SIRPA, IL23A, IL1B, OSM, OLR1, KLRC2, CXCR6, IL17RA, KLRC1, ADAM10 and TNF; or [epithelial cells] CTSA, TNIP1, SEPHS2, AGPAT2, MIDN, FAM132A, SLC26A3, CHP2, SULT1A2, TMEM171, SULTIA1, Clorf106, HNF4A, PLEKHG6, FUT2, CEBPA, GSDMB, EDN3, PTK6, PSORSICI, RHPN2, VDR, SLC26A6, AGPAT3, MST1R, NGEF, EFNA2, C2CD2L, ITPKA, SLC22A5, SLC35D1, AGXT, NXPE4, SLC39A8, TMEM258, F12, D2HGDH, BCL2L15, CFTR, GOT1, PLK1, ERGICI, ITLN1, REG4, SULT2B1, CCDCl₆₀, CACNA2D2, SLC19A3, AGFG2, PLXNB1, DDC, C2orf54, LFNG, SNAPC4, MEX3A, GCG, GPBAR1, RXFP4, UCKL1, HCK, CAMP, BLM, SOX4, IFT172, RNF186, SMURF1, RNF123, TREH, HOXA11-AS, NOS2, C2CD4D, CEBPG, IL10RB, PRKCD, MED16, SEC16A, PPP1R12C, FOXO1, EPS8L1, TRIM31, CDH1, APOBR, SCNN1A, GRB7, SLC22A23, FRYL, ACHE, SMAD3, MAGI3, SPRED2, SMPD3, FAM83E, IL1R2, USP12, PWP2, ABCA7, SYT7 and COG5. Thus, cells may be targeted that express GWAS genes.

In another aspect, the present invention provides for an isolated gastrointestinal tract cell characterized by expression of one or markers for a cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12.

In another aspect, the present invention provides for a method for detecting or quantifying gastrointestinal tract cells in a biological sample of a subject, the method comprising detecting or quantifying in the biological sample gastrointestinal tract cells as defined in any embodiment herein. The gastrointestinal tract cell may be detected or quantified using one or more markers for a cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12.

In another aspect, the present invention provides for a method of isolating a gastrointestinal tract cell from a biological sample of a subject, the method comprising isolating from the biological sample gastrointestinal tract cells as defined as defined in any embodiment herein. The gastrointestinal tract cell may be isolated using one or more surface markers for a cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12.

In certain embodiments, the gastrointestinal tract cells may be isolated, detected or quantified using a technique selected from the group consisting of RT-PCR, RNA-seq, single cell RNA-seq, western blot, ELISA, flow cytometry, mass cytometry, fluorescence activated cell sorting, fluorescence microscopy, affinity separation, magnetic cell separation, microfluidic separation, and combinations thereof.

In another aspect, the present invention provides for a method of modulating the gastrointestinal tract cell composition comprising treating a subject with an agent capable of targeting intestinal stem cells to differentiate. The intestinal stem cells may be targeted to differentiate into absorptive transit amplifying (TA) 1 cells, absorptive TA 2 cells or class switching B cells.

In another aspect, the present invention provides for a method of modulating the gastrointestinal tract cell composition or activity comprising treating a subject with an agent capable of targeting a receptor-ligand interaction. The receptor-ligand interaction may comprise: CCR7 and one or more of CCL19 and CCL21; TNFB and LTBR; LGR5 and RSPO3; IL15 and IL15RA; FGF23 and FGFR1; CCL8 and CCR1; CXCL2 and XCR1; or XCL2 and XCR1.

In certain embodiments, IBD comprises Crohn's disease or ulcerative colitis (UC).

In another aspect, the present invention provides for a method of detecting drug resistance in inflammatory bowel disease (IBD) comprising measuring in a biological sample obtained from the gastrointestinal tract of a subject the frequency of colitis-associated inflammatory fibroblasts (CAIFs) compared to the total of all cell types in the sample, wherein drug resistance is detected when the frequency of CAIFs is altered as compared to a healthy frequency. The drug resistance may be resistance to anti-TNF therapy. The cell type may be detected by measuring one or markers selected from the group consisting of MMP3, MMP10, PLAU, IL1R1, IL13RA2, CXCL6, CCL11, TNFSF11 and TNFRSF11B.

These and other aspects, objects, features, and advantages of the example embodiments will become apparent to those having ordinary skill in the art upon consideration of the following detailed description of illustrated example embodiments.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1—illustrates that epithelial cells in UC patients partition by patient and healthy cells by cell type in tSNE plots.

FIG. 2—illustrates that computational modeling can address batch effects in tSNE plots.

FIG. 3—illustrates that the atlas uncovers almost all cell types and subtypes in the colon.

FIG. 4—illustrates that the atlas uncovers almost all immune cell types and subtypes in the colon.

FIG. 5—illustrates the changes in cellular composition in UC.

FIG. 6—illustrates that the atlas can be used to analyze compositional changes by deconvolution of bulk profiles.

FIG. 7—illustrates genes differentially expressed in UC.

FIG. 8—illustrates cell type specific differential expression of genes in UC.

FIG. 9—illustrates genes differentially expressed in uninflamed tissue and in inflamed tissue.

FIG. 10—illustrates violin plots for key IBD GWAS in specific cell types present in healthy and disease colon.

FIG. 11—illustrates violin plots for key IBD GWAS in specific cell types present in healthy and disease colon.

FIG. 12—illustrates the cell-of-origin for key IBD GWAS genes.

FIG. 13—illustrates the cell-of-origin for key IBD GWAS genes. Gene modules for all cells and TA cells are specific for an epithelial cell signature and oxidative phosphorylation signature.

FIG. 14—illustrates the cell-of-origin for key IBD GWAS G-protein coupled receptor (GPCR) genes.

FIG. 15—illustrates the cell-of-origin for key IBD GWAS cell-cell interaction or cell-cell communication genes.

FIG. 16—illustrates the cell-of-origin for key IBD GWAS genes expressed in epithelial cells.

FIG. 17—illustrates that the atlas can be used to determine the cell-of-origin for GWAS genes for other indications.

FIG. 18—illustrates that the atlas can be used to determine cell-cell interaction mechanisms.

FIG. 19—illustrates cell-cell interactions in the healthy gut.

FIG. 20—illustrates cell-cell interactions in the diseased gut.

FIG. 21—illustrates that the atlas can be used to determine fibroblasts that support the stem cell niche.

FIG. 22—illustrates fibroblasts genes that support the stem cell niche. (right) BMP expression and Wnt expression in the villus and crypt.

FIG. 23—illustrates Rspo3 gene expression in the tSNE plot of FIG. 22.

FIG. 24—illustrates a Rspo3 gene expression module and a module from all cells in the tSNE plot.

FIG. 25—illustrates a diagram of the study design and sample collection.

FIG. 26—Cell atlas of the human colon in health and disease. a. tSNE clustering by cell type. b. Heatmap showing expression of cell type specific markers. c. Barplot showing proportions of cell subsets across samples of the same type (health, uninflamed, inflamed). d. Plot showing distribution of cell types. e. Expression of novel markers in cell subsets. f. Expression of specific markers in cell subsets. g. Pathway showing that angiotensinogen is produced by WNT5B+ fibroblasts, renin by BEST4+ enterocytes, Angiotensin Converting Enzyme (ACE) by epithelial and endothelial cells, and the angiotensin receptor AGTR1 by WNT2B+ fibroblasts and pericytes. h. Heatmap showing expression of cell type specific markers.

FIG. 27—Shifts in Cell Populations in UC. a. cell frequencies across samples. b. distribution of “pseudotime” values along each of the absorptive and secretory branches. c. general epithelial markers for inflamed cells. d. general innate immune markers for inflamed cells. e. general adaptive immune markers for inflamed cells. f. specific epithelial markers for inflamed cells. g. specific innate immune markers for inflamed cells. h. specific adaptive immune markers for inflamed cells. i. cell frequencies across samples. i. cell frequencies across samples.

FIG. 28—Inflammatory pathways. a. Violin plots showing expression of IL-17, cytotoxicity, and co-inhibiotory signatures in healthy, non-inflamed and inflamed samples. b. Heatmaps comparing cytokines between inflamed tissue, non-inflamed tissue and healthy tissue. c. Anti-TNF violin plots. Plot showing fold change of TNF signaling. d. TNF signature compared to the drug resistance signature and drug susceptibility signature in cell subsets. e. heatmap showing changes in the expression of pathways related to nutrient sensing, stress, and inflammation across all cell types. f. Expression of drug resistance signature genes in subsets.

FIG. 29—Cell-Cell Network Rewiring and GWAS. a. Healthy cell-cell network. b. Non-inflamed cell-cell network c. Inflamed cell-cell network. d. shows ligand expression correlated with the frequency of the cells expressing its cognate receptor. e. LASSO regression analysis to predict the frequency of each cell subset using the expression levels of all cognate ligands of its receptors in other cells.

FIG. 30—a. Heatmap of 53 IBD-associated GWAS genes onto the colon cell atlas. b,c. plot comparing GWAS expression in subsets for healthy and inflamed cells.

FIG. 31—Barplots showing the fraction of cells in the samples.

FIG. 32—Heatmap showing expression of transcription factors across all cells, healthy cells and UC cells.

FIG. 33—Heatmap showing expression of G protein-coupled receptors (GPRC) across all cells, healthy cells and UC cells.

FIG. 34—Heatmap showing expression of transporters across all cells, healthy cells and UC cells.

FIG. 35—Heatmap showing expression of cytokines across all cells, healthy cells and UC cells.

FIG. 36—Heatmap showing expression of pattern recognition receptors (PRR) across all cells, healthy cells and UC cells.

FIG. 37—Univariate analysis (with Fisher's exact test) on each cell frequency.

FIG. 38—illustrates IgG class switching in healthy and inflamed tissues.

FIG. 39—a. Volcano plot showing general epithelial markers for uninflamed cells. b. Volcano plot showing general fibroblast markers for uninflamed cells. c. Volcano plot showing general immune markers for uninflamed cells. d. Volcano plot showing cell specific epithelial markers for uninflamed cells. e. Volcano plot showing cell specific fibroblast markers for uninflamed cells. f. Volcano plot showing cell specific immune markers for uninflamed cells.

FIG. 40—Most cell intrinsic expression changes in UC are shared between inflamed and uninflamed regions. a. general pan compartment and subset specific epithelial markers for inflamed and uninflamed cells. b. general pan compartment and subset specific stroma markers for inflamed and uninflamed cells. c. general pan compartment and subset specific immune markers for inflamed and uninflamed cells.

FIG. 41—A shift in TNF source to CAIF may underlie resistance to anti-TNF therapy. a. Plot showing fold change of TNF signaling. b. anti-TNF violin plots.

DETAILED DESCRIPTION OF THE EXAMPLE EMBODIMENTS General Definitions

Unless defined otherwise, technical and scientific terms used herein have the same meaning as commonly understood by one of ordinary skill in the art to which this disclosure pertains. Definitions of common terms and techniques in molecular biology may be found in Molecular Cloning: A Laboratory Manual, 2^(nd) edition (1989) (Sambrook, Fritsch, and Maniatis); Molecular Cloning: A Laboratory Manual, 4^(th) edition (2012) (Green and Sambrook); Current Protocols in Molecular Biology (1987) (F. M. Ausubel et al. eds.); the series Methods in Enzymology (Academic Press, Inc.): PCR 2: A Practical Approach (1995) (M. J. MacPherson, B. D. Hames, and G. R. Taylor eds.): Antibodies, A Laboraotry Manual (1988) (Harlow and Lane, eds.): Antibodies A Laboraotry Manual, 2^(nd) edition 2013 (E. A. Greenfield ed.); Animal Cell Culture (1987) (R. I. Freshney, ed.); Benjamin Lewin, Genes IX, published by Jones and Bartlet, 2008 (ISBN 0763752223); Kendrew et al. (eds.), The Encyclopedia of Molecular Biology, published by Blackwell Science Ltd., 1994 (ISBN 0632021829); Robert A. Meyers (ed.), Molecular Biology and Biotechnology: a Comprehensive Desk Reference, published by VCH Publishers, Inc., 1995 (ISBN 9780471185710); Singleton et al., Dictionary of Microbiology and Molecular Biology 2nd ed., J. Wiley & Sons (New York, N.Y. 1994), March, Advanced Organic Chemistry Reactions, Mechanisms and Structure 4th ed., John Wiley & Sons (New York, N.Y. 1992); and Marten H. Hofker and Jan van Deursen, Transgenic Mouse Methods and Protocols, 2^(nd) edition (2011).

As used herein, the singular forms “a”, “an”, and “the” include both singular and plural referents unless the context clearly dictates otherwise.

The term “optional” or “optionally” means that the subsequent described event, circumstance or substituent may or may not occur, and that the description includes instances where the event or circumstance occurs and instances where it does not.

The recitation of numerical ranges by endpoints includes all numbers and fractions subsumed within the respective ranges, as well as the recited endpoints.

The terms “about” or “approximately” as used herein when referring to a measurable value such as a parameter, an amount, a temporal duration, and the like, are meant to encompass variations of and from the specified value, such as variations of +/−10% or less, +/−5% or less, +/−1% or less, and +/−0.1% or less of and from the specified value, insofar such variations are appropriate to perform in the disclosed invention. It is to be understood that the value to which the modifier “about” or “approximately” refers is itself also specifically, and preferably, disclosed.

Reference throughout this specification to “one embodiment”, “an embodiment,” “an example embodiment,” means that a particular feature, structure or characteristic described in connection with the embodiment is included in at least one embodiment of the present invention. Thus, appearances of the phrases “in one embodiment,” “in an embodiment,” or “an example embodiment” in various places throughout this specification are not necessarily all referring to the same embodiment, but may. Furthermore, the particular features, structures or characteristics may be combined in any suitable manner, as would be apparent to a person skilled in the art from this disclosure, in one or more embodiments. Furthermore, while some embodiments described herein include some but not other features included in other embodiments, combinations of features of different embodiments are meant to be within the scope of the invention. For example, in the appended claims, any of the claimed embodiments can be used in any combination.

All publications, published patent documents, and patent applications cited in this application are indicative of the level of skill in the art(s) to which the application pertains. All publications, published patent documents, and patent applications cited herein are hereby incorporated by reference to the same extent as though each individual publication, published patent document, or patent application was specifically and individually indicated as being incorporated by reference.

Overview

Embodiments disclosed herein provide for a human cell atlas of the colon from healthy and diseased subjects. Applicants identified additional phenotypic markers for these cells in the lamina propria and addressed the role of these location-specific regulatory cells in the prevention and the resolution of intestinal inflammation in human UC. The atlas was obtained by single sequencing of about 117,819 cells. By sequencing single cells from biopsies that are routinely collected during the treatment of IBD, Applicants were able to generate complete molecular profiles of the disease within each patient at single cell resolution. This single cell census of the human colon during health and disease revealed nearly all disease-relevant cell types, with the notable exception of neutrophils, and will serve as a foundational resource for the scientific community. Surprisingly, the analysis revealed new cell types and states in the colon, including a subset of chemosensory epithelial cells that may detect pH and contribute to sour taste perception in the colon, and several disease-specific cell subsets whose contributions to IBD were largely unknown, including M cells, CAIFs, inflammatory monocytes, and CD8⁺IL-17⁺ T cells. The analysis provides a framework for using sc-RNA-Seq to understand complex diseases: first, mapping cell types and cell states within healthy and diseased tissue, identifying changes in cell proportions with disease, and partitioning changes in gene expression into those that are shared by cell lineages or unique to cell subsets; then, integrating these analyses to understand how changes in gene expression propagate into changes in cell-cell interactions, identifying the “cell-of-action” for GWAS genes, and understanding the complex genetic risk factors for the disease.

The present invention discloses novel markers for cell types. Moreover, genes associated with disease are identified in the colon and colon specific cell types. The invention provides for diagnostic assays based on gene markers and cell composition, as well as target cell types that express genes associated with disease. The invention provides for modulating cell types and cell-cell interactions in the gut (e.g., for treating IBD). Finally, disclosed are novel cell types and methods of quantitating, detecting and isolating the cell types

Biomarkers and Signatures

The invention further relates to various biomarkers for quantitating, detecting or isolating gut cell subpopulations. The populations may be detected by detecting one or more biomarkers in a sample.

The term “biomarker” is widespread in the art and commonly broadly denotes a biological molecule, more particularly an endogenous biological molecule, and/or a detectable portion thereof, whose qualitative and/or quantitative evaluation in a tested object (e.g., in or on a cell, cell population, tissue, organ, or organism, e.g., in a biological sample of a subject) is predictive or informative with respect to one or more aspects of the tested object's phenotype and/or genotype. The terms “marker” and “biomarker” may be used interchangeably throughout this specification. Biomarkers as intended herein may be nucleic acid-based or peptide-, polypeptide- and/or protein-based. For example, a marker may be comprised of peptide(s), polypeptide(s) and/or protein(s) encoded by a given gene, or of detectable portions thereof. Further, whereas the term “nucleic acid” generally encompasses DNA, RNA and DNA/RNA hybrid molecules, in the context of markers the term may typically refer to heterogeneous nuclear RNA (hnRNA), pre-mRNA, messenger RNA (mRNA), or complementary DNA (cDNA), or detectable portions thereof. Such nucleic acid species are particularly useful as markers, since they contain qualitative and/or quantitative information about the expression of the gene. Particularly preferably, a nucleic acid-based marker may encompass mRNA of a given gene, or cDNA made of the mRNA, or detectable portions thereof. Any such nucleic acid(s), peptide(s), polypeptide(s) and/or protein(s) encoded by or produced from a given gene are encompassed by the term “gene product(s)”.

Preferably, markers as intended herein may be extracellular or cell surface markers, as methods to measure extracellular or cell surface marker(s) need not disturb the integrity of the cell membrane and may not require fixation/permeabilization of the cells.

Unless otherwise apparent from the context, reference herein to any marker, such as a peptide, polypeptide, protein, or nucleic acid, may generally also encompass modified forms of said marker, such as bearing post-expression modifications including, for example, phosphorylation, glycosylation, lipidation, methylation, cysteinylation, sulphonation, glutathionylation, acetylation, oxidation of methionine to methionine sulphoxide or methionine sulphone, and the like.

The term “peptide” as used throughout this specification preferably refers to a polypeptide as used herein consisting essentially of 50 amino acids or less, e.g., 45 amino acids or less, preferably 40 amino acids or less, e.g., 35 amino acids or less, more preferably 30 amino acids or less, e.g., 25 or less, 20 or less, 15 or less, 10 or less or 5 or less amino acids.

The term “polypeptide” as used throughout this specification generally encompasses polymeric chains of amino acid residues linked by peptide bonds. Hence, insofar a protein is only composed of a single polypeptide chain, the terms “protein” and “polypeptide” may be used interchangeably herein to denote such a protein. The term is not limited to any minimum length of the polypeptide chain. The term may encompass naturally, recombinantly, semi-synthetically or synthetically produced polypeptides. The term also encompasses polypeptides that carry one or more co- or post-expression-type modifications of the polypeptide chain, such as, without limitation, glycosylation, acetylation, phosphorylation, sulfonation, methylation, ubiquitination, signal peptide removal, N-terminal Met removal, conversion of pro-enzymes or pre-hormones into active forms, etc. The term further also includes polypeptide variants or mutants which carry amino acid sequence variations vis-à-vis a corresponding native polypeptide, such as, e.g., amino acid deletions, additions and/or substitutions. The term contemplates both full-length polypeptides and polypeptide parts or fragments, e.g., naturally-occurring polypeptide parts that ensue from processing of such full-length polypeptides.

The term “protein” as used throughout this specification generally encompasses macromolecules comprising one or more polypeptide chains, i.e., polymeric chains of amino acid residues linked by peptide bonds. The term may encompass naturally, recombinantly, semi-synthetically or synthetically produced proteins. The term also encompasses proteins that carry one or more co- or post-expression-type modifications of the polypeptide chain(s), such as, without limitation, glycosylation, acetylation, phosphorylation, sulfonation, methylation, ubiquitination, signal peptide removal, N-terminal Met removal, conversion of pro-enzymes or pre-hormones into active forms, etc. The term further also includes protein variants or mutants which carry amino acid sequence variations vis-à-vis a corresponding native protein, such as, e.g., amino acid deletions, additions and/or substitutions. The term contemplates both full-length proteins and protein parts or fragments, e.g., naturally-occurring protein parts that ensue from processing of such full-length proteins.

The reference to any marker, including any peptide, polypeptide, protein, or nucleic acid, corresponds to the marker commonly known under the respective designations in the art. The terms encompass such markers of any organism where found, and particularly of animals, preferably warm-blooded animals, more preferably vertebrates, yet more preferably mammals, including humans and non-human mammals, still more preferably of humans.

The terms particularly encompass such markers, including any peptides, polypeptides, proteins, or nucleic acids, with a native sequence, i.e., ones of which the primary sequence is the same as that of the markers found in or derived from nature. A skilled person understands that native sequences may differ between different species due to genetic divergence between such species. Moreover, native sequences may differ between or within different individuals of the same species due to normal genetic diversity (variation) within a given species. Also, native sequences may differ between or even within different individuals of the same species due to somatic mutations, or post-transcriptional or post-translational modifications. Any such variants or isoforms of markers are intended herein. Accordingly, all sequences of markers found in or derived from nature are considered “native”. The terms encompass the markers when forming a part of a living organism, organ, tissue or cell, when forming a part of a biological sample, as well as when at least partly isolated from such sources. The terms also encompass markers when produced by recombinant or synthetic means.

In certain embodiments, markers, including any peptides, polypeptides, proteins, or nucleic acids, may be human, i.e., their primary sequence may be the same as a corresponding primary sequence of or present in a naturally occurring human markers. Hence, the qualifier “human” in this connection relates to the primary sequence of the respective markers, rather than to their origin or source. For example, such markers may be present in or isolated from samples of human subjects or may be obtained by other means (e.g., by recombinant expression, cell-free transcription or translation, or non-biological nucleic acid or peptide synthesis).

The reference herein to any marker, including any peptide, polypeptide, protein, or nucleic acid, also encompasses fragments thereof. Hence, the reference herein to measuring (or measuring the quantity of) any one marker may encompass measuring the marker and/or measuring one or more fragments thereof.

For example, any marker and/or one or more fragments thereof may be measured collectively, such that the measured quantity corresponds to the sum amounts of the collectively measured species. In another example, any marker and/or one or more fragments thereof may be measured each individually. The terms encompass fragments arising by any mechanism, in vivo and/or in vitro, such as, without limitation, by alternative transcription or translation, exo- and/or endo-proteolysis, exo- and/or endo-nucleolysis, or degradation of the peptide, polypeptide, protein, or nucleic acid, such as, for example, by physical, chemical and/or enzymatic proteolysis or nucleolysis.

The term “fragment” as used throughout this specification with reference to a peptide, polypeptide, or protein generally denotes a portion of the peptide, polypeptide, or protein, such as typically an N- and/or C-terminally truncated form of the peptide, polypeptide, or protein. Preferably, a fragment may comprise at least about 30%, e.g., at least about 50% or at least about 70%, preferably at least about 80%, e.g., at least about 85%, more preferably at least about 90%, and yet more preferably at least about 95% or even about 99% of the amino acid sequence length of said peptide, polypeptide, or protein. For example, insofar not exceeding the length of the full-length peptide, polypeptide, or protein, a fragment may include a sequence of ≥5 consecutive amino acids, or ≥10 consecutive amino acids, or ≥20 consecutive amino acids, or ≥30 consecutive amino acids, e.g., ≥40 consecutive amino acids, such as for example ≥50 consecutive amino acids, e.g., ≥60, ≥70, ≥80, ≥90, ≥100, ≥200, ≥300, ≥400, ≥500 or ≥600 consecutive amino acids of the corresponding full-length peptide, polypeptide, or protein.

The term “fragment” as used throughout this specification with reference to a nucleic acid (polynucleotide) generally denotes a 5′- and/or 3′-truncated form of a nucleic acid. Preferably, a fragment may comprise at least about 30%, e.g., at least about 50% or at least about 70%, preferably at least about 80%, e.g., at least about 85%, more preferably at least about 90%, and yet more preferably at least about 95% or even about 99% of the nucleic acid sequence length of said nucleic acid. For example, insofar not exceeding the length of the full-length nucleic acid, a fragment may include a sequence of ≥5 consecutive nucleotides, or ≥10 consecutive nucleotides, or ≥20 consecutive nucleotides, or ≥30 consecutive nucleotides, e.g., ≥40 consecutive nucleotides, such as for example ≥50 consecutive nucleotides, e.g., ≥60, ≥70, ≥80, ≥90, ≥100, ≥200, ≥300, ≥400, ≥500 or ≥600 consecutive nucleotides of the corresponding full-length nucleic acid.

Cells such as immune cells as disclosed herein may in the context of the present specification be said to “comprise the expression” or conversely to “not express” one or more markers, such as one or more genes or gene products; or be described as “positive” or conversely as “negative” for one or more markers, such as one or more genes or gene products; or be said to “comprise” a defined “gene or gene product signature”.

Such terms are commonplace and well-understood by the skilled person when characterizing cell phenotypes. By means of additional guidance, when a cell is said to be positive for or to express or comprise expression of a given marker, such as a given gene or gene product, a skilled person would conclude the presence or evidence of a distinct signal for the marker when carrying out a measurement capable of detecting or quantifying the marker in or on the cell. Suitably, the presence or evidence of the distinct signal for the marker would be concluded based on a comparison of the measurement result obtained for the cell to a result of the same measurement carried out for a negative control (for example, a cell known to not express the marker) and/or a positive control (for example, a cell known to express the marker). Where the measurement method allows for a quantitative assessment of the marker, a positive cell may generate a signal for the marker that is at least 1.5-fold higher than a signal generated for the marker by a negative control cell or than an average signal generated for the marker by a population of negative control cells, e.g., at least 2-fold, at least 4-fold, at least 10-fold, at least 20-fold, at least 30-fold, at least 40-fold, at least 50-fold higher or even higher. Further, a positive cell may generate a signal for the marker that is 3.0 or more standard deviations, e.g., 3.5 or more, 4.0 or more, 4.5 or more, or 5.0 or more standard deviations, higher than an average signal generated for the marker by a population of negative control cells.

The present invention is also directed to signatures and uses thereof. As used herein a “signature” may encompass any gene or genes, protein or proteins, or epigenetic element(s) whose expression profile or whose occurrence is associated with a specific cell type, subtype, or cell state of a specific cell type or subtype within a population of cells (e.g., tumor infiltrating lymphocytes). In certain embodiments, the expression of the CD8⁺ TIL signatures are dependent on epigenetic modification of the genes or regulatory elements associated with the genes. Thus, in certain embodiments, use of signature genes includes epigenetic modifications that may be detected or modulated. For ease of discussion, when discussing gene expression, any gene or genes, protein or proteins, or epigenetic element(s) may be substituted. Reference to a gene name throughout the specification encompasses the human gene, mouse gene and all other orthologues as known in the art in other organisms. As used herein, the terms “signature”, “expression profile”, or “expression program” may be used interchangeably. It is to be understood that also when referring to proteins (e.g. differentially expressed proteins), such may fall within the definition of “gene” signature. Levels of expression or activity or prevalence may be compared between different cells in order to characterize or identify for instance signatures specific for cell (sub)populations. Increased or decreased expression or activity of signature genes may be compared between different cells in order to characterize or identify for instance specific cell (sub)populations. The detection of a signature in single cells may be used to identify and quantitate for instance specific cell (sub)populations. A signature may include a gene or genes, protein or proteins, or epigenetic element(s) whose expression or occurrence is specific to a cell (sub)population, such that expression or occurrence is exclusive to the cell (sub)population. A gene signature as used herein, may thus refer to any set of up- and down-regulated genes that are representative of a cell type or subtype. A gene signature as used herein, may also refer to any set of up- and down-regulated genes between different cells or cell (sub)populations derived from a gene-expression profile. For example, a gene signature may comprise a list of genes differentially expressed in a distinction of interest.

The signature as defined herein (being it a gene signature, protein signature or other genetic or epigenetic signature) can be used to indicate the presence of a cell type, a subtype of the cell type, the state of the microenvironment of a population of cells, a particular cell type population or subpopulation, and/or the overall status of the entire cell (sub)population. Furthermore, the signature may be indicative of cells within a population of cells in vivo. The signature may also be used to suggest for instance particular therapies, or to follow up treatment, or to suggest ways to modulate immune systems. The signatures of the present invention may be discovered by analysis of expression profiles of single-cells within a population of cells from isolated samples (e.g. tumor samples), thus allowing the discovery of novel cell subtypes or cell states that were previously invisible or unrecognized. The presence of subtypes or cell states may be determined by subtype specific or cell state specific signatures. The presence of these specific cell (sub)types or cell states may be determined by applying the signature genes to bulk sequencing data in a sample. Not being bound by a theory the signatures of the present invention may be microenvironment specific, such as their expression in a particular spatio-temporal context. Not being bound by a theory, signatures as discussed herein are specific to a particular pathological context. Not being bound by a theory, a combination of cell subtypes having a particular signature may indicate an outcome. Not being bound by a theory, the signatures can be used to deconvolute the network of cells present in a particular pathological condition. Not being bound by a theory the presence of specific cells and cell subtypes are indicative of a particular response to treatment, such as including increased or decreased susceptibility to treatment. The signature may indicate the presence of one particular cell type.

The signature according to certain embodiments of the present invention may comprise or consist of one or more genes, proteins and/or epigenetic elements, such as for instance 1, 2, 3, 4, 5, 6, 7, 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of two or more genes, proteins and/or epigenetic elements, such as for instance 2, 3, 4, 5, 6, 7, 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of three or more genes, proteins and/or epigenetic elements, such as for instance 3, 4, 5, 6, 7, 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of four or more genes, proteins and/or epigenetic elements, such as for instance 4, 5, 6, 7, 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of five or more genes, proteins and/or epigenetic elements, such as for instance 5, 6, 7, 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of six or more genes, proteins and/or epigenetic elements, such as for instance 6, 7, 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of seven or more genes, proteins and/or epigenetic elements, such as for instance 7, 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of eight or more genes, proteins and/or epigenetic elements, such as for instance 8, 9, 10 or more. In certain embodiments, the signature may comprise or consist of nine or more genes, proteins and/or epigenetic elements, such as for instance 9, 10 or more. In certain embodiments, the signature may comprise or consist of ten or more genes, proteins and/or epigenetic elements, such as for instance 10, 11, 12, 13, 14, 15, or more. It is to be understood that a signature according to the invention may for instance also include genes or proteins as well as epigenetic elements combined.

In certain embodiments, a signature is characterized as being specific for a particular cell or cell (sub)population state if it is upregulated or only present, detected or detectable in that particular cell or cell (sub)population state (e.g., disease or healthy), or alternatively is downregulated or only absent, or undetectable in that particular cell or cell (sub)population state. In this context, a signature consists of one or more differentially expressed genes/proteins or differential epigenetic elements when comparing different cells or cell (sub)populations, including comparing different gut cell or gut cell (sub)populations, as well as comparing gut cell or gut cell (sub)populations with healthy or disease (sub)populations. It is to be understood that “differentially expressed” genes/proteins include genes/proteins which are up- or down-regulated as well as genes/proteins which are turned on or off. When referring to up-or down-regulation, in certain embodiments, such up- or down-regulation is preferably at least two-fold, such as two-fold, three-fold, four-fold, five-fold, or more, such as for instance at least ten-fold, at least 20-fold, at least 30-fold, at least 40-fold, at least 50-fold, or more. Alternatively, or in addition, differential expression may be determined based on common statistical tests, as is known in the art.

As discussed herein, differentially expressed genes/proteins, or differential epigenetic elements may be differentially expressed on a single cell level, or may be differentially expressed on a cell population level. Preferably, the differentially expressed genes/proteins or epigenetic elements as discussed herein, such as constituting the gene signatures as discussed herein, when as to the cell population or subpopulation level, refer to genes that are differentially expressed in all or substantially all cells of the population or subpopulation (such as at least 80%, preferably at least 90%, such as at least 95% of the individual cells). This allows one to define a particular subpopulation of immune cells. As referred to herein, a “subpopulation” of cells preferably refers to a particular subset of cells of a particular cell type which can be distinguished or are uniquely identifiable and set apart from other cells of this cell type. The cell subpopulation may be phenotypically characterized, and is preferably characterized by the signature as discussed herein. A cell (sub)population as referred to herein may constitute of a (sub)population of cells of a particular cell type characterized by a specific cell state.

When referring to induction, or alternatively suppression of a particular signature, preferable is meant induction or alternatively suppression (or upregulation or downregulation) of at least one gene/protein and/or epigenetic element of the signature, such as for instance at least two, at least three, at least four, at least five, at least six, or all genes/proteins and/or epigenetic elements of the signature.

Various aspects and embodiments of the invention may involve analyzing gene signatures, protein signature, and/or other genetic or epigenetic signature based on single cell analyses (e.g. single cell RNA sequencing) or alternatively based on cell population analyses, as is defined herein elsewhere.

In certain example embodiments, the signature genes may be used to deconvolute the network of cells present in a tumor based on comparing them to data from bulk analysis of a tumor sample. In certain example embodiments, the presence of specific immune cells and immune cell subtypes may be indicative of tumor growth, invasiveness and/or resistance to treatment. In one example embodiment, detection of one or more signature genes may indicate the presence of a particular cell type or cell types. In certain example embodiments, the presence of immune cell types within a tumor may indicate that the tumor will be sensitive to a treatment (e.g., checkpoint blockade therapy). In one embodiment, the signature genes of the present invention are applied to bulk sequencing data from a tumor sample obtained from a subject, such that information relating to disease outcome and personalized treatments is determined.

Detection of Gut Cell Sub-Populations

In one embodiment, the method comprises detecting or quantifying gut cells in a biological sample obtained from the gastrointestinal tract (e.g., colon, intestine). A marker, for example a gene or gene product, for example a peptide, polypeptide, protein, or nucleic acid, or a group of two or more markers, is “detected” or “measured” in a tested object (e.g., in or on a cell, cell population, tissue, organ, or organism, e.g., in a biological sample of a subject) when the presence or absence and/or quantity of said marker or said group of markers is detected or determined in the tested object, preferably substantially to the exclusion of other molecules and analytes, e.g., other genes or gene products.

The terms “increased” or “increase” or “upregulated” or “upregulate” as used herein generally mean an increase by a statically significant amount. For avoidance of doubt, “increased” means a statistically significant increase of at least 10% as compared to a reference level, including an increase of at least 20%, at least 30%, at least 40%, at least 50%, at least 60%, at least 70%, at least 80%, at least 90%, at least 100% or more, including, for example at least 2-fold, at least 3-fold, at least 4-fold, at least 5-fold, at least 10-fold increase or greater as compared to a reference level, as that term is defined herein.

The term “reduced” or “reduce” or “decrease” or “decreased” or “downregulate” or “downregulated” as used herein generally means a decrease by a statistically significant amount relative to a reference. For avoidance of doubt, “reduced” means statistically significant decrease of at least 10% as compared to a reference level, for example a decrease by at least 20%, at least 30%, at least 40%, at least 50%, or at least 60%, or at least 70%, or at least 80%, at least 90% or more, up to and including a 100% decrease (i.e., absent level as compared to a reference sample), or any decrease between 10-100% as compared to a reference level, as that.

The terms “sample” or “biological sample” as used throughout this specification include any biological specimen obtained from a subject. Particularly useful samples are those known to comprise, or expected or predicted to comprise gut cells as taught herein. Preferably, a sample may be readily obtainable by minimally invasive methods, such as blood collection or tissue biopsy, allowing the removal/isolation/provision of the sample from the subject (e.g., colonoscopy).

The terms “quantity”, “amount” and “level” are synonymous and generally well-understood in the art. The terms as used throughout this specification may particularly refer to an absolute quantification of a marker in a tested object (e.g., in or on a cell, cell population, tissue, organ, or organism, e.g., in a biological sample of a subject), or to a relative quantification of a marker in a tested object, i.e., relative to another value such as relative to a reference value, or to a range of values indicating a base-line of the marker. Such values or ranges may be obtained as conventionally known.

An absolute quantity of a marker may be advantageously expressed as weight or as molar amount, or more commonly as a concentration, e.g., weight per volume or mol per volume. A relative quantity of a marker may be advantageously expressed as an increase or decrease or as a fold-increase or fold-decrease relative to said another value, such as relative to a reference value. Performing a relative comparison between first and second variables (e.g., first and second quantities) may but need not require determining first the absolute values of said first and second variables. For example, a measurement method may produce quantifiable readouts (such as, e.g., signal intensities) for said first and second variables, wherein said readouts are a function of the value of said variables, and wherein said readouts may be directly compared to produce a relative value for the first variable vs. the second variable, without the actual need to first convert the readouts to absolute values of the respective variables.

Reference values may be established according to known procedures previously employed for other cell populations, biomarkers and gene or gene product signatures. For example, a reference value may be established in an individual or a population of individuals characterized by a particular diagnosis, prediction and/or prognosis of said disease or condition (i.e., for whom said diagnosis, prediction and/or prognosis of the disease or condition holds true). Such population may comprise without limitation 2 or more, 10 or more, 100 or more, or even several hundred or more individuals.

A “deviation” of a first value from a second value may generally encompass any direction (e.g., increase: first value >second value; or decrease: first value <second value) and any extent of alteration.

For example, a deviation may encompass a decrease in a first value by, without limitation, at least about 10% (about 0.9-fold or less), or by at least about 20% (about 0.8-fold or less), or by at least about 30% (about 0.7-fold or less), or by at least about 40% (about 0.6-fold or less), or by at least about 50% (about 0.5-fold or less), or by at least about 60% (about 0.4-fold or less), or by at least about 70% (about 0.3-fold or less), or by at least about 80% (about 0.2-fold or less), or by at least about 90% (about 0.1-fold or less), relative to a second value with which a comparison is being made.

For example, a deviation may encompass an increase of a first value by, without limitation, at least about 10% (about 1.1-fold or more), or by at least about 20% (about 1.2-fold or more), or by at least about 30% (about 1.3-fold or more), or by at least about 40% (about 1.4-fold or more), or by at least about 50% (about 1.5-fold or more), or by at least about 60% (about 1.6-fold or more), or by at least about 70% (about 1.7-fold or more), or by at least about 80% (about 1.8-fold or more), or by at least about 90% (about 1.9-fold or more), or by at least about 100% (about 2-fold or more), or by at least about 150% (about 2.5-fold or more), or by at least about 200% (about 3-fold or more), or by at least about 500% (about 6-fold or more), or by at least about 700% (about 8-fold or more), or like, relative to a second value with which a comparison is being made.

Preferably, a deviation may refer to a statistically significant observed alteration. For example, a deviation may refer to an observed alteration which falls outside of error margins of reference values in a given population (as expressed, for example, by standard deviation or standard error, or by a predetermined multiple thereof, e.g., ±1×SD or ±2×SD or ±3×SD, or 1×SE or ±2×SE or ±3×SE). Deviation may also refer to a value falling outside of a reference range defined by values in a given population (for example, outside of a range which comprises ≥40%, ≥50%, ≥60%, ≥70%, ≥75% or ≥80% or ≥85% or ≥90% or ≥95% or even ≥100% of values in said population).

In a further embodiment, a deviation may be concluded if an observed alteration is beyond a given threshold or cut-off. Such threshold or cut-off may be selected as generally known in the art to provide for a chosen sensitivity and/or specificity of the prediction methods, e.g., sensitivity and/or specificity of at least 50%, or at least 60%, or at least 70%, or at least 80%, or at least 85%, or at least 90%, or at least 95%.

For example, receiver-operating characteristic (ROC) curve analysis can be used to select an optimal cut-off value of the quantity of a given immune cell population, biomarker or gene or gene product signatures, for clinical use of the present diagnostic tests, based on acceptable sensitivity and specificity, or related performance measures which are well-known per se, such as positive predictive value (PPV), negative predictive value (NPV), positive likelihood ratio (LR+), negative likelihood ratio (LR−), Youden index, or similar.

The terms “diagnosis” and “monitoring” are commonplace and well-understood in medical practice. By means of further explanation and without limitation the term “diagnosis” generally refers to the process or act of recognizing, deciding on or concluding on a disease or condition in a subject on the basis of symptoms and signs and/or from results of various diagnostic procedures (such as, for example, from knowing the presence, absence and/or quantity of one or more biomarkers characteristic of the diagnosed disease or condition).

The term “monitoring” generally refers to the follow-up of a disease or a condition in a subject for any changes which may occur over time.

The terms “prognosing” or “prognosis” generally refer to an anticipation on the progression of a disease or condition and the prospect (e.g., the probability, duration, and/or extent) of recovery. A good prognosis of the diseases or conditions taught herein may generally encompass anticipation of a satisfactory partial or complete recovery from the diseases or conditions, preferably within an acceptable time period. A good prognosis of such may more commonly encompass anticipation of not further worsening or aggravating of such, preferably within a given time period. A poor prognosis of the diseases or conditions as taught herein may generally encompass anticipation of a substandard recovery and/or unsatisfactorily slow recovery, or to substantially no recovery or even further worsening of such.

The terms also encompass prediction of a disease. The terms “predicting” or “prediction” generally refer to an advance declaration, indication or foretelling of a disease or condition in a subject not (yet) having said disease or condition. For example, a prediction of a disease or condition in a subject may indicate a probability, chance or risk that the subject will develop said disease or condition, for example within a certain time period or by a certain age. Said probability, chance or risk may be indicated inter alia as an absolute value, range or statistics, or may be indicated relative to a suitable control subject or subject population (such as, e.g., relative to a general, normal or healthy subject or subject population). Hence, the probability, chance or risk that a subject will develop a disease or condition may be advantageously indicated as increased or decreased, or as fold-increased or fold-decreased relative to a suitable control subject or subject population. As used herein, the term “prediction” of the conditions or diseases as taught herein in a subject may also particularly mean that the subject has a ‘positive’ prediction of such, i.e., that the subject is at risk of having such (e.g., the risk is significantly increased vis-à-vis a control subject or subject population). The term “prediction of no” diseases or conditions as taught herein as described herein in a subject may particularly mean that the subject has a ‘negative’ prediction of such, i.e., that the subject's risk of having such is not significantly increased vis-à-vis a control subject or subject population.

Methods of Detection and Isolation of Cell Types Using Biomarkers

In certain embodiments, the gut cell types may be detected, quantified or isolated using a technique selected from the group consisting of flow cytometry, mass cytometry, fluorescence activated cell sorting (FACS), fluorescence microscopy, affinity separation, magnetic cell separation, microfluidic separation, RNA-seq (e.g., bulk or single cell), quantitative PCR, MERFISH (multiplex (in situ) RNA FISH) and combinations thereof. The technique may employ one or more agents capable of specifically binding to one or more gene products expressed or not expressed by the gut cells, preferably on the cell surface of the gut cells. The one or more agents may be one or more antibodies. Other methods including absorbance assays and colorimetric assays are known in the art and may be used herein.

Depending on factors that can be evaluated and decided on by a skilled person, such as, inter alia, the type of a marker (e.g., peptide, polypeptide, protein, or nucleic acid), the type of the tested object (e.g., a cell, cell population, tissue, organ, or organism, e.g., the type of biological sample of a subject, e.g., whole blood, plasma, serum, tissue biopsy), the expected abundance of the marker in the tested object, the type, robustness, sensitivity and/or specificity of the detection method used to detect the marker, etc., the marker may be measured directly in the tested object, or the tested object may be subjected to one or more processing steps aimed at achieving an adequate measurement of the marker.

In other example embodiments, detection of a marker may include immunological assay methods, wherein the ability of an assay to separate, detect and/or quantify a marker (such as, preferably, peptide, polypeptide, or protein) is conferred by specific binding between a separable, detectable and/or quantifiable immunological binding agent (antibody) and the marker. Immunological assay methods include without limitation immunohistochemistry, immunocytochemistry, flow cytometry, mass cytometry, fluorescence activated cell sorting (FACS), fluorescence microscopy, fluorescence based cell sorting using microfluidic systems, immunoaffinity adsorption based techniques such as affinity chromatography, magnetic particle separation, magnetic activated cell sorting or bead based cell sorting using microfluidic systems, enzyme-linked immunosorbent assay (ELISA) and ELISPOT based techniques, radioimmunoassay (RIA), Western blot, etc.

In certain example embodiments, detection of a marker or signature may include biochemical assay methods, including inter alia assays of enzymatic activity, membrane channel activity, substance-binding activity, gene regulatory activity, or cell signaling activity of a marker, e.g., peptide, polypeptide, protein, or nucleic acid.

In other example embodiments, detection of a marker may include mass spectrometry analysis methods. Generally, any mass spectrometric (MS) techniques that are capable of obtaining precise information on the mass of peptides, and preferably also on fragmentation and/or (partial) amino acid sequence of selected peptides (e.g., in tandem mass spectrometry, MS/MS; or in post source decay, TOF MS), may be useful herein for separation, detection and/or quantification of markers (such as, preferably, peptides, polypeptides, or proteins). Suitable peptide MS and MS/MS techniques and systems are well-known per se (see, e.g., Methods in Molecular Biology, vol. 146: “Mass Spectrometry of Proteins and Peptides”, by Chapman, ed., Humana Press 2000, ISBN 089603609x; Biemann 1990. Methods Enzymol 193: 455-79; or Methods in Enzymology, vol. 402: “Biological Mass Spectrometry”, by Burlingame, ed., Academic Press 2005, ISBN 9780121828073) and may be used herein. MS arrangements, instruments and systems suitable for biomarker peptide analysis may include, without limitation, matrix-assisted laser desorption/ionisation time-of-flight (MALDI-TOF) MS; MALDI-TOF post-source-decay (PSD); MALDI-TOF/TOF; surface-enhanced laser desorption/ionization time-of-flight mass spectrometry (SELDI-TOF) MS; electrospray ionization mass spectrometry (ESI-MS); ESI-MS/MS; ESI-MS/(MS)n (n is an integer greater than zero); ESI 3D or linear (2D) ion trap MS; ESI triple quadrupole MS; ESI quadrupole orthogonal TOF (Q-TOF); ESI Fourier transform MS systems; desorption/ionization on silicon (DIOS); secondary ion mass spectrometry (SIMS); atmospheric pressure chemical ionization mass spectrometry (APCI-MS); APCI-MS/MS; APCI-(MS)n; atmospheric pressure photoionization mass spectrometry (APPI-MS); APPI-MS/MS; and APPI-(MS)n. Peptide ion fragmentation in tandem MS (MS/MS) arrangements may be achieved using manners established in the art, such as, e.g., collision induced dissociation (CID). Detection and quantification of markers by mass spectrometry may involve multiple reaction monitoring (MRM), such as described among others by Kuhn et al. 2004 (Proteomics 4: 1175-86). MS peptide analysis methods may be advantageously combined with upstream peptide or protein separation or fractionation methods, such as for example with the chromatographic and other methods.

In other example embodiments, detection of a marker may include chromatography methods. In a one example embodiment, chromatography refers to a process in which a mixture of substances (analytes) carried by a moving stream of liquid or gas (“mobile phase”) is separated into components as a result of differential distribution of the analytes, as they flow around or over a stationary liquid or solid phase (“stationary phase”), between said mobile phase and said stationary phase. The stationary phase may be usually a finely divided solid, a sheet of filter material, or a thin film of a liquid on the surface of a solid, or the like. Chromatography may be columnar. While particulars of chromatography are well known in the art, for further guidance see, e.g., Meyer M., 1998, ISBN: 047198373X, and “Practical HPLC Methodology and Applications”, Bidlingmeyer, B. A., John Wiley & Sons Inc., 1993. Exemplary types of chromatography include, without limitation, high-performance liquid chromatography (HPLC), normal phase HPLC (NP-HPLC), reversed phase HPLC (RP-HPLC), ion exchange chromatography (IEC), such as cation or anion exchange chromatography, hydrophilic interaction chromatography (HILIC), hydrophobic interaction chromatography (HIC), size exclusion chromatography (SEC) including gel filtration chromatography or gel permeation chromatography, chromatofocusing, affinity chromatography such as immunoaffinity, immobilised metal affinity chromatography, and the like.

In certain embodiments, further techniques for separating, detecting and/or quantifying markers may be used in conjunction with any of the above described detection methods. Such methods include, without limitation, chemical extraction partitioning, isoelectric focusing (IEF) including capillary isoelectric focusing (CIEF), capillary isotachophoresis (CITP), capillary electrochromatography (CEC), and the like, one-dimensional polyacrylamide gel electrophoresis (PAGE), two-dimensional polyacrylamide gel electrophoresis (2D-PAGE), capillary gel electrophoresis (CGE), capillary zone electrophoresis (CZE), micellar electrokinetic chromatography (MEKC), free flow electrophoresis (FFE), etc.

In certain examples, such methods may include separating, detecting and/or quantifying markers at the nucleic acid level, more particularly RNA level, e.g., at the level of hnRNA, pre-mRNA, mRNA, or cDNA. Standard quantitative RNA or cDNA measurement tools known in the art may be used. Non-limiting examples include hybridization-based analysis, microarray expression analysis, digital gene expression profiling (DGE), RNA-in-situ hybridization (RISH), Northern-blot analysis and the like; PCR, RT-PCR, RT-qPCR, end-point PCR, digital PCR or the like; supported oligonucleotide detection, pyrosequencing, polony cyclic sequencing by synthesis, simultaneous bi-directional sequencing, single-molecule sequencing, single molecule real time sequencing, true single molecule sequencing, hybridization-assisted nanopore sequencing, sequencing by synthesis, single-cell RNA sequencing (sc-RNA seq), or the like. By means of an example, methods to profile the RNA content of large numbers of individual cells have been recently developed.

In certain embodiments, the invention involves plate based single cell RNA sequencing (see, e.g., Picelli, S. et al., 2014, “Full-length RNA-seq from single cells using Smart-seq2” Nature protocols 9, 171-181, doi:10.1038/nprot.2014.006).

In certain embodiments, special microfluidic devices have been developed to encapsulate each cell in an individual drop, associate the RNA of each cell with a ‘cell barcode’ unique to that cell/drop, measure the expression level of each RNA with sequencing, and then use the cell barcodes to determine which cell each RNA molecule came from. In certain embodiments, single cells are segregated. In these regards, reference is made to Macosko et al., 2015, “Highly Parallel Genome-wide Expression Profiling of Individual Cells Using Nanoliter Droplets” Cell 161, 1202-1214; International patent application number PCT/US2015/049178, published as WO2016/040476 on Mar. 17, 2016; Klein et al., 2015, “Droplet Barcoding for Single-Cell Transcriptomics Applied to Embryonic Stem Cells” Cell 161, 1187-1201; International patent application number PCT/US2016/027734, published as WO2016168584A1 on Oct. 20, 2016; Zheng, et al., 2016, “Haplotyping germline and cancer genomes with high-throughput linked-read sequencing” Nature Biotechnology 34, 303-311; Zheng, et al., 2017, “Massively parallel digital transcriptional profiling of single cells” Nat. Commun. 8, 14049 doi: 10.1038/ncomms14049; International patent publication number WO2014210353A2; Zilionis, et al., 2017, “Single-cell barcoding and sequencing using droplet microfluidics” Nat Protoc. January; 12(1):44-73; Cao et al., 2017, “Comprehensive single cell transcriptional profiling of a multicellular organism by combinatorial indexing” bioRxiv preprint first posted online Feb. 2, 2017, doi: dx.doi.org/10.1101/104844; Rosenberg et al., 2017, “Scaling single cell transcriptomics through split pool barcoding” bioRxiv preprint first posted online Feb. 2, 2017, doi: dx.doi.org/10.1101/105163; Vitak, et al., “Sequencing thousands of single-cell genomes with combinatorial indexing” Nature Methods, 14(3):302-308, 2017; Cao, et al., Comprehensive single-cell transcriptional profiling of a multicellular organism. Science, 357(6352):661-667, 2017; and Gierahn et al., “Seq-Well: portable, low-cost RNA sequencing of single cells at high throughput” Nature Methods 14, 395-398 (2017), all the contents and disclosure of each of which are herein incorporated by reference in their entirety.

In certain embodiments, the invention involves single nucleus RNA sequencing. In this regard reference is made to Swiech et al., 2014, “In vivo interrogation of gene function in the mammalian brain using CRISPR-Cas9” Nature Biotechnology Vol. 33, pp. 102-106; Habib et al., 2016, “Div-Seq: Single-nucleus RNA-Seq reveals dynamics of rare adult newborn neurons” Science, Vol. 353, Issue 6302, pp. 925-928; Habib et al., 2017, “Massively parallel single-nucleus RNA-seq with DroNc-seq” Nat Methods. 2017 October; 14(10):955-958; and International patent application number PCT/US2016/059239, published as WO2017164936 on Sep. 28, 2017, which are herein incorporated by reference in their entirety.

The terms “isolating” or “purifying” as used throughout this specification with reference to a particular component of a composition or mixture (e.g., the tested object such as the biological sample) encompass processes or techniques whereby such component is separated from one or more or (substantially) all other components of the composition or mixture (e.g., the tested object such as the biological sample). The terms do not require absolute purity. Instead, isolating or purifying the component will produce a discrete environment in which the abundance of the component relative to one or more or all other components is greater than in the starting composition or mixture (e.g., the tested object such as the biological sample). A discrete environment may denote a single medium, such as for example a single solution, dispersion, gel, precipitate, etc. Isolating or purifying the specified cells from the tested object such as the biological sample may increase the abundance of the specified cells relative to all other cells comprised in the tested object such as the biological sample, or relative to other cells of a select subset of the cells comprised in the tested object such as the biological sample, e.g., relative to other white blood cells, peripheral blood mononuclear cells, immune cells, antigen presenting cells, or dendritic cells comprised in the tested object such as the biological sample. By means of example, isolating or purifying the specified cells from the tested object such as the biological sample may yield a cell population, in which the specified cells constitute at least 40% (by number) of all cells of said cell population, for example, at least 45%, preferably at least 50%, at least 55%, more preferably at least 60%, at least 65%, still more preferably at least 70%, at least 75%, even more preferably at least 80%, at least 85%, and yet more preferably at least 90%, at least 95%, at least 96%, at least 97%, at least 98%, at least 99%, or even 100% of all cells of said cell population.

The method may allow to detect or conclude the presence or absence of the specified cells in a tested object (e.g., in a cell population, tissue, organ, organism, or in a biological sample of a subject). The method may also allow to quantify the specified cells in a tested object (e.g., in a cell population, tissue, organ, organism, or in a biological sample of a subject). The quantity of the specified cells in the tested object such as the biological sample may be suitably expressed for example as the number (count) of the specified immune cells per standard unit of volume (e.g., ml, μl or nl) or weight (e.g., g or mg or ng) of the tested object such as the biological sample. The quantity of the specified cells in the tested object such as the biological sample may also be suitably expressed as a percentage or fraction (by number) of all cells comprised in the tested object such as the biological sample, or as a percentage or fraction (by number) of a select subset of the cells comprised in the tested object such as the biological sample, e.g., as a percentage or fraction (by number) of white blood cells, peripheral blood mononuclear cells, immune cells, antigen presenting cells, or dendritic cells comprised in the tested object such as the biological sample. The quantity of the specified cells in the tested object such as the biological sample may also be suitably represented by an absolute or relative quantity of a suitable surrogate analyte, such as a peptide, polypeptide, protein, or nucleic acid expressed or comprised by the specified cells.

Where a marker is detected in or on a cell, the cell may be conventionally denoted as positive (+) or negative (−) for the marker. Semi-quantitative denotations of marker expression in cells are also commonplace in the art, such as particularly in flow cytometry quantifications, for example, “dim” vs. “bright”, or “low” vs. “medium”/“intermediate” vs. “high”, or “−” vs. “+” vs. “+*”, commonly controlled in flow cytometry quantifications by setting of the gates. Where a marker is quantified in or on a cell, absolute quantity of the marker may also be expressed for example as the number of molecules of the marker comprised by the cell.

Where a marker is detected and/or quantified on a single cell level in a cell population, the quantity of the marker may also be expressed as a percentage or fraction (by number) of cells comprised in said population that are positive for said marker, or as percentages or fractions (by number) of cells comprised in said population that are “dim” or “bright”, or that are “low” or “medium”/“intermediate” or “high”, or that are “−” or “+” or “+*”. By means of an example, a sizeable proportion of the tested cells of the cell population may be positive for the marker, e.g., at least about 20%, at least about 40%, at least about 50%, at least about 60%, at least about 70%, at least about 80%, at least about 90%, at least about 95%, or up to 100%.

Use of Specific Binding Agents

In certain embodiments, the aforementioned methods and techniques may employ agent(s) capable of specifically binding to one or more gene products, e.g., peptides, polypeptides, proteins, or nucleic acids, expressed or not expressed by the immune cells as taught herein. In certain preferred embodiments, such one or more gene products, e.g., peptides, polypeptides, or proteins, may be expressed on the cell surface of the immune cells (i.e., cell surface markers, e.g., transmembrane peptides, polypeptides or proteins, or secreted peptides, polypeptides or proteins which remain associated with the cell surface). Hence, further disclosed are binding agents capable of specifically binding to markers, such as genes or gene products, e.g., peptides, polypeptides, proteins, or nucleic acids as taught herein. Binding agents as intended throughout this specification may include inter alia antibodies, aptamers, spiegelmers (L-aptamers), photoaptamers, protein, peptides, peptidomimetics, nucleic acids such as oligonucleotides (e.g., hybridization probes or amplification or sequencing primers and primer pairs), small molecules, or combinations thereof.

The term “aptamer” refers to single-stranded or double-stranded oligo-DNA, oligo-RNA or oligo-DNA/RNA or any analogue thereof that specifically binds to a target molecule such as a peptide. Advantageously, aptamers display fairly high specificity and affinity (e.g., KA in the order 1×109 M−1) for their targets. Aptamer production is described inter alia in U.S. Pat. No. 5,270,163; Ellington & Szostak 1990 (Nature 346: 818-822); Tuerk & Gold 1990 (Science 249: 505-510); or “The Aptamer Handbook: Functional Oligonucleotides and Their Applications”, by Klussmann, ed., Wiley-VCH 2006, ISBN 3527310592, incorporated by reference herein. The term “photoaptamer” refers to an aptamer that contains one or more photoreactive functional groups that can covalently bind to or crosslink with a target molecule. The term “spiegelmer” refers to an aptamer which includes L-DNA, L-RNA, or other left-handed nucleotide derivatives or nucleotide-like molecules. Aptamers containing left-handed nucleotides are resistant to degradation by naturally occurring enzymes, which normally act on substrates containing right-handed nucleotides. The term “peptidomimetic” refers to a non-peptide agent that is a topological analogue of a corresponding peptide. Methods of rationally designing peptidomimetics of peptides are known in the art. For example, the rational design of three peptidomimetics based on the sulphated 8-mer peptide CCK26-33, and of two peptidomimetics based on the 11-mer peptide Substance P, and related peptidomimetic design principles, are described in Horwell 1995 (Trends Biotechnol 13: 132-134).

Binding agents may be in various forms, e.g., lyophilised, free in solution, or immobilised on a solid phase. They may be, e.g., provided in a multi-well plate or as an array or microarray, or they may be packaged separately, individually, or in combination.

The term “specifically bind” as used throughout this specification means that an agent (denoted herein also as “specific-binding agent”) binds to one or more desired molecules or analytes (e.g., peptides, polypeptides, proteins, or nucleic acids) substantially to the exclusion of other molecules which are random or unrelated, and optionally substantially to the exclusion of other molecules that are structurally related. The term “specifically bind” does not necessarily require that an agent binds exclusively to its intended target(s). For example, an agent may be said to specifically bind to target(s) of interest if its affinity for such intended target(s) under the conditions of binding is at least about 2-fold greater, preferably at least about 5-fold greater, more preferably at least about 10-fold greater, yet more preferably at least about 25-fold greater, still more preferably at least about 50-fold greater, and even more preferably at least about 100-fold, or at least about 1000-fold, or at least about 104-fold, or at least about 105-fold, or at least about 106-fold or more greater, than its affinity for a non-target molecule, such as for a suitable control molecule (e.g., bovine serum albumin, casein).

Preferably, the specific binding agent may bind to its intended target(s) with affinity constant (KA) of such binding KA≥1×106 M−1, more preferably KA≥1×107 M−1, yet more preferably KA≥1×108 M−1, even more preferably KA≥1×109 M−1, and still more preferably KA 1×1010 M−1 or KA 1×1011 M−1 or KA≥1×1012 M−1, wherein KA=[SBA_T]/[SBA][T], SBA denotes the specific-binding agent, T denotes the intended target. Determination of KA can be carried out by methods known in the art, such as for example, using equilibrium dialysis and Scatchard plot analysis.

In certain embodiments, the one or more binding agents may be one or more antibodies. As used herein, the term “antibody” is used in its broadest sense and generally refers to any immunologic binding agent. The term specifically encompasses intact monoclonal antibodies, polyclonal antibodies, multivalent (e.g., 2-, 3- or more-valent) and/or multi-specific antibodies (e.g., bi- or more-specific antibodies) formed from at least two intact antibodies, and antibody fragments insofar they exhibit the desired biological activity (particularly, ability to specifically bind an antigen of interest, i.e., antigen-binding fragments), as well as multivalent and/or multi-specific composites of such fragments. The term “antibody” is not only inclusive of antibodies generated by methods comprising immunization, but also includes any polypeptide, e.g., a recombinantly expressed polypeptide, which is made to encompass at least one complementarity-determining region (CDR) capable of specifically binding to an epitope on an antigen of interest. Hence, the term applies to such molecules regardless whether they are produced in vitro or in vivo. Antibodies also encompasses chimeric, humanized and fully humanized antibodies.

An antibody may be any of IgA, IgD, IgE, IgG and IgM classes, and preferably IgG class antibody. An antibody may be a polyclonal antibody, e.g., an antiserum or immunoglobulins purified there from (e.g., affinity-purified). An antibody may be a monoclonal antibody or a mixture of monoclonal antibodies. Monoclonal antibodies can target a particular antigen or a particular epitope within an antigen with greater selectivity and reproducibility. By means of example and not limitation, monoclonal antibodies may be made by the hybridoma method first described by Kohler et al. 1975 (Nature 256: 495), or may be made by recombinant DNA methods (e.g., as in U.S. Pat. No. 4,816,567). Monoclonal antibodies may also be isolated from phage antibody libraries using techniques as described by Clackson et al. 1991 (Nature 352: 624-628) and Marks et al. 1991 (J Mol Biol 222: 581-597), for example.

Antibody binding agents may be antibody fragments. “Antibody fragments” comprise a portion of an intact antibody, comprising the antigen-binding or variable region thereof. Examples of antibody fragments include Fab, Fab′, F(ab′)2, Fv and scFv fragments, single domain (sd) Fv, such as VH domains, VL domains and VHH domains; diabodies; linear antibodies; single-chain antibody molecules, in particular heavy-chain antibodies; and multivalent and/or multispecific antibodies formed from antibody fragment(s), e.g., dibodies, tribodies, and multibodies. The above designations Fab, Fab′, F(ab′)2, Fv, scFv etc. are intended to have their art-established meaning.

The term antibody includes antibodies originating from or comprising one or more portions derived from any animal species, preferably vertebrate species, including, e.g., birds and mammals. Without limitation, the antibodies may be chicken, turkey, goose, duck, guinea fowl, quail or pheasant. Also without limitation, the antibodies may be human, murine (e.g., mouse, rat, etc.), donkey, rabbit, goat, sheep, guinea pig, camel (e.g., Camelus bactrianus and Camelus dromaderius), llama (e.g., Lama paccos, Lama glama or Lama vicugna) or horse.

A skilled person will understand that an antibody can include one or more amino acid deletions, additions and/or substitutions (e.g., conservative substitutions), insofar such alterations preserve its binding of the respective antigen. An antibody may also include one or more native or artificial modifications of its constituent amino acid residues (e.g., glycosylation, etc.).

Methods of producing polyclonal and monoclonal antibodies as well as fragments thereof are well known in the art, as are methods to produce recombinant antibodies or fragments thereof (see for example, Harlow and Lane, “Antibodies: A Laboratory Manual”, Cold Spring Harbour Laboratory, New York, 1988; Harlow and Lane, “Using Antibodies: A Laboratory Manual”, Cold Spring Harbour Laboratory, New York, 1999, ISBN 0879695447; “Monoclonal Antibodies: A Manual of Techniques”, by Zola, ed., CRC Press 1987, ISBN 0849364760; “Monoclonal Antibodies: A Practical Approach”, by Dean & Shepherd, eds., Oxford University Press 2000, ISBN 0199637229; Methods in Molecular Biology, vol. 248: “Antibody Engineering: Methods and Protocols”, Lo, ed., Humana Press 2004, ISBN 1588290921).

As used herein, a “blocking” antibody or an antibody “antagonist” is one which inhibits or reduces biological activity of the antigen(s) it binds. In certain embodiments, the blocking antibodies or antagonist antibodies or portions thereof described herein completely inhibit the biological activity of the antigen(s).

Antibodies may act as agonists or antagonists of the recognized polypeptides. For example, the present invention includes antibodies which disrupt receptor/ligand interactions either partially or fully. The invention features both receptor-specific antibodies and ligand-specific antibodies. The invention also features receptor-specific antibodies which do not prevent ligand binding but prevent receptor activation. Receptor activation (i.e., signaling) may be determined by techniques described herein or otherwise known in the art. For example, receptor activation can be determined by detecting the phosphorylation (e.g., tyrosine or serine/threonine) of the receptor or of one of its down-stream substrates by immunoprecipitation followed by western blot analysis. In specific embodiments, antibodies are provided that inhibit ligand activity or receptor activity by at least 95%, at least 90%, at least 85%, at least 80%, at least 75%, at least 70%, at least 60%, or at least 50% of the activity in absence of the antibody.

The invention also features receptor-specific antibodies which both prevent ligand binding and receptor activation as well as antibodies that recognize the receptor-ligand complex. Likewise, encompassed by the invention are neutralizing antibodies which bind the ligand and prevent binding of the ligand to the receptor, as well as antibodies which bind the ligand, thereby preventing receptor activation, but do not prevent the ligand from binding the receptor. Further included in the invention are antibodies which activate the receptor. These antibodies may act as receptor agonists, i.e., potentiate or activate either all or a subset of the biological activities of the ligand-mediated receptor activation, for example, by inducing dimerization of the receptor. The antibodies may be specified as agonists, antagonists or inverse agonists for biological activities comprising the specific biological activities of the peptides disclosed herein. The antibody agonists and antagonists can be made using methods known in the art. See, e.g., PCT publication WO 96/40281; U.S. Pat. No. 5,811,097; Deng et al., Blood 92(6):1981-1988 (1998); Chen et al., Cancer Res. 58(16):3668-3678 (1998); Harrop et al., J. Immunol. 161(4):1786-1794 (1998); Zhu et al., Cancer Res. 58(15):3209-3214 (1998); Yoon et al., J. Immunol. 160(7):3170-3179 (1998); Prat et al., J. Cell. Sci. III (Pt2):237-247 (1998); Pitard et al., J. Immunol. Methods 205(2):177-190 (1997); Liautard et al., Cytokine 9(4):233-241 (1997); Carlson et al., J. Biol. Chem. 272(17):11295-11301 (1997); Taryman et al., Neuron 14(4):755-762 (1995); Muller et al., Structure 6(9):1153-1167 (1998); Bartunek et al., Cytokine 8(1):14-20 (1996).

The antibodies as defined for the present invention include derivatives that are modified, i.e., by the covalent attachment of any type of molecule to the antibody such that covalent attachment does not prevent the antibody from generating an anti-idiotypic response. For example, but not by way of limitation, the antibody derivatives include antibodies that have been modified, e.g., by glycosylation, acetylation, pegylation, phosphylation, amidation, derivatization by known protecting/blocking groups, proteolytic cleavage, linkage to a cellular ligand or other protein, etc. Any of numerous chemical modifications may be carried out by known techniques, including, but not limited to specific chemical cleavage, acetylation, formylation, metabolic synthesis of tunicamycin, etc. Additionally, the derivative may contain one or more non-classical amino acids.

Simple binding assays can be used to screen for or detect agents that bind to a target protein, or disrupt the interaction between proteins (e.g., a receptor and a ligand). Because certain targets of the present invention are transmembrane proteins, assays that use the soluble forms of these proteins rather than full-length protein can be used, in some embodiments. Soluble forms include, for example, those lacking the transmembrane domain and/or those comprising the IgV domain or fragments thereof which retain their ability to bind their cognate binding partners. Further, agents that inhibit or enhance protein interactions for use in the compositions and methods described herein, can include recombinant peptido-mimetics.

Detection methods useful in screening assays include antibody-based methods, detection of a reporter moiety, detection of cytokines as described herein, and detection of a gene signature as described herein.

Another variation of assays to determine binding of a receptor protein to a ligand protein is through the use of affinity biosensor methods. Such methods may be based on the piezoelectric effect, electrochemistry, or optical methods, such as ellipsometry, optical wave guidance, and surface plasmon resonance (SPR).

The term “antibody-like protein scaffolds” or “engineered protein scaffolds” broadly encompasses proteinaceous non-immunoglobulin specific-binding agents, typically obtained by combinatorial engineering (such as site-directed random mutagenesis in combination with phage display or other molecular selection techniques). Usually, such scaffolds are derived from robust and small soluble monomeric proteins (such as Kunitz inhibitors or lipocalins) or from a stably folded extra-membrane domain of a cell surface receptor (such as protein A, fibronectin or the ankyrin repeat).

Such scaffolds have been extensively reviewed in Binz et al. (Engineering novel binding proteins from nonimmunoglobulin domains. Nat Biotechnol 2005, 23:1257-1268), Gebauer and Skerra (Engineered protein scaffolds as next-generation antibody therapeutics. Curr Opin Chem Biol. 2009, 13:245-55), Gill and Damle (Biopharmaceutical drug discovery using novel protein scaffolds. Curr Opin Biotechnol 2006, 17:653-658), Skerra (Engineered protein scaffolds for molecular recognition. J Mol Recognit 2000, 13:167-187), and Skerra (Alternative non-antibody scaffolds for molecular recognition. Curr Opin Biotechnol 2007, 18:295-304), and include without limitation affibodies, based on the Z-domain of staphylococcal protein A, a three-helix bundle of 58 residues providing an interface on two of its alpha-helices (Nygren, Alternative binding proteins: Affibody binding proteins developed from a small three-helix bundle scaffold. FEBS J 2008, 275:2668-2676); engineered Kunitz domains based on a small (ca. 58 residues) and robust, disulphide-crosslinked serine protease inhibitor, typically of human origin (e.g. LACI-D1), which can be engineered for different protease specificities (Nixon and Wood, Engineered protein inhibitors of proteases. Curr Opin Drug Discov Dev 2006, 9:261-268); monobodies or adnectins based on the 10th extracellular domain of human fibronectin III (10Fn3), which adopts an Ig-like beta-sandwich fold (94 residues) with 2-3 exposed loops, but lacks the central disulphide bridge (Koide and Koide, Monobodies: antibody mimics based on the scaffold of the fibronectin type III domain. Methods Mol Biol 2007, 352:95-109); anticalins derived from the lipocalins, a diverse family of eight-stranded beta-barrel proteins (ca. 180 residues) that naturally form binding sites for small ligands by means of four structurally variable loops at the open end, which are abundant in humans, insects, and many other organisms (Skerra, Alternative binding proteins: Anticalins-harnessing the structural plasticity of the lipocalin ligand pocket to engineer novel binding activities. FEBS J 2008, 275:2677-2683); DARPins, designed ankyrin repeat domains (166 residues), which provide a rigid interface arising from typically three repeated beta-turns (Stumpp et al., DARPins: a new generation of protein therapeutics. Drug Discov Today 2008, 13:695-701); avimers (multimerized LDLR-A module) (Silverman et al., Multivalent avimer proteins evolved by exon shuffling of a family of human receptor domains. Nat Biotechnol 2005, 23:1556-1561); and cysteine-rich knottin peptides (Kolmar, Alternative binding proteins: biological activity and therapeutic potential of cystine-knot miniproteins. FEBS J 2008, 275:2684-2690).

Nucleic acid binding agents, such as oligonucleotide binding agents, are typically at least partly antisense to a target nucleic acid of interest. The term “antisense” generally refers to an agent (e.g., an oligonucleotide) configured to specifically anneal with (hybridise to) a given sequence in a target nucleic acid, such as for example in a target DNA, hnRNA, pre-mRNA or mRNA, and typically comprises, consist essentially of or consist of a nucleic acid sequence that is complementary or substantially complementary to said target nucleic acid sequence. Antisense agents suitable for use herein, such as hybridisation probes or amplification or sequencing primers and primer pairs) may typically be capable of annealing with (hybridizing to) the respective target nucleic acid sequences at high stringency conditions, and capable of hybridising specifically to the target under physiological conditions. The terms “complementary” or “complementarity” as used throughout this specification with reference to nucleic acids, refer to the normal binding of single-stranded nucleic acids under permissive salt (ionic strength) and temperature conditions by base pairing, preferably Watson-Crick base pairing. By means of example, complementary Watson-Crick base pairing occurs between the bases A and T, A and U or G and C. For example, the sequence 5′-A-G-U-3′ is complementary to sequence 5′-A-C-U-3′.

The reference to oligonucleotides may in particular but without limitation include hybridization probes and/or amplification primers and/or sequencing primers, etc., as commonly used in nucleic acid detection technologies.

Binding agents as discussed herein may suitably comprise a detectable label. The term “label” refers to any atom, molecule, moiety or biomolecule that may be used to provide a detectable and preferably quantifiable read-out or property, and that may be attached to or made part of an entity of interest, such as a binding agent. Labels may be suitably detectable by for example mass spectrometric, spectroscopic, optical, colourimetric, magnetic, photochemical, biochemical, immunochemical or chemical means. Labels include without limitation dyes; radiolabels such as ³²P, ³³P, ³⁵S, ¹²⁵I, ¹³¹I; electron-dense reagents; enzymes (e.g., horse-radish peroxidase or alkaline phosphatase as commonly used in immunoassays); binding moieties such as biotin-streptavidin; haptens such as digoxigenin; luminogenic, phosphorescent or fluorogenic moieties; mass tags; and fluorescent dyes alone or in combination with moieties that may suppress or shift emission spectra by fluorescence resonance energy transfer (FRET).

In some embodiments, binding agents may be provided with a tag that permits detection with another agent (e.g., with a probe binding partner). Such tags may be, for example, biotin, streptavidin, his-tag, myc tag, maltose, maltose binding protein or any other kind of tag known in the art that has a binding partner. Example of associations which may be utilised in the probe:binding partner arrangement may be any, and includes, for example biotin:streptavidin, his-tag:metal ion (e.g., Ni2⁺), maltose:maltose binding protein, etc.

The marker-binding agent conjugate may be associated with or attached to a detection agent to facilitate detection. Examples of detection agents include, but are not limited to, luminescent labels; colourimetric labels, such as dyes; fluorescent labels; or chemical labels, such as electroactive agents (e.g., ferrocyanide); enzymes; radioactive labels; or radiofrequency labels. The detection agent may be a particle. Examples of such particles include, but are not limited to, colloidal gold particles; colloidal sulphur particles; colloidal selenium particles; colloidal barium sulfate particles; colloidal iron sulfate particles; metal iodate particles; silver halide particles; silica particles; colloidal metal (hydrous) oxide particles; colloidal metal sulfide particles; colloidal lead selenide particles; colloidal cadmium selenide particles; colloidal metal phosphate particles; colloidal metal ferrite particles; any of the above-mentioned colloidal particles coated with organic or inorganic layers; protein or peptide molecules; liposomes; or organic polymer latex particles, such as polystyrene latex beads. Preferable particles may be colloidal gold particles.

In certain embodiments, the one or more binding agents are configured for use in a technique selected from the group consisting of flow cytometry, fluorescence activated cell sorting, mass cytometry, fluorescence microscopy, affinity separation, magnetic cell separation, microfluidic separation, and combinations thereof.

Identifying Modulators

A further aspect of the invention relates to a method for identifying an agent capable of modulating one or more phenotypic aspects of a gut cell or gut cell population as disclosed herein, comprising: a) applying a candidate agent to the cell or cell population; b) detecting modulation of one or more phenotypic aspects of the cell or cell population by the candidate agent, thereby identifying the agent.

The term “modulate” broadly denotes a qualitative and/or quantitative alteration, change or variation in that which is being modulated. Where modulation can be assessed quantitatively—for example, where modulation comprises or consists of a change in a quantifiable variable such as a quantifiable property of a cell or where a quantifiable variable provides a suitable surrogate for the modulation—modulation specifically encompasses both increase (e.g., activation) or decrease (e.g., inhibition) in the measured variable. The term encompasses any extent of such modulation, e.g., any extent of such increase or decrease, and may more particularly refer to statistically significant increase or decrease in the measured variable. By means of example, modulation may encompass an increase in the value of the measured variable by at least about 10%, e.g., by at least about 20%, preferably by at least about 30%, e.g., by at least about 40%, more preferably by at least about 50%, e.g., by at least about 75%, even more preferably by at least about 100%, e.g., by at least about 150%, 200%, 250%, 300%, 400% or by at least about 500%, compared to a reference situation without said modulation; or modulation may encompass a decrease or reduction in the value of the measured variable by at least about 10%, e.g., by at least about 20%, by at least about 30%, e.g., by at least about 40%, by at least about 50%, e.g., by at least about 60%, by at least about 70%, e.g., by at least about 80%, by at least about 90%, e.g., by at least about 95%, such as by at least about 96%, 97%, 98%, 99% or even by 100%, compared to a reference situation without said modulation. Preferably, modulation may be specific or selective, hence, one or more desired phenotypic aspects of a gut cell or gut cell population may be modulated without substantially altering other (unintended, undesired) phenotypic aspect(s).

The term “agent” broadly encompasses any condition, substance or agent capable of modulating one or more phenotypic aspects of an gut cell or gut cell population as disclosed herein. Such conditions, substances or agents may be of physical, chemical, biochemical and/or biological nature. The term “candidate agent” refers to any condition, substance or agent that is being examined for the ability to modulate one or more phenotypic aspects of an gut cell or gut cell population as disclosed herein in a method comprising applying the candidate agent to the gut cell or gut cell population (e.g., exposing the gut cell or gut cell population to the candidate agent or contacting the gut cell or gut cell population with the candidate agent) and observing whether the desired modulation takes place.

Agents may include any potential class of biologically active conditions, substances or agents, such as for instance antibodies, proteins, peptides, nucleic acids, oligonucleotides, small molecules, or combinations thereof.

By means of example but without limitation, agents can include low molecular weight compounds, but may also be larger compounds, or any organic or inorganic molecule effective in the given situation, including modified and unmodified nucleic acids such as antisense nucleic acids, RNAi, such as siRNA or shRNA, CRISPR/Cas systems, peptides, peptidomimetics, receptors, ligands, and antibodies, aptamers, polypeptides, nucleic acid analogues or variants thereof. Examples include an oligomer of nucleic acids, amino acids, or carbohydrates including without limitation proteins, oligonucleotides, ribozymes, DNAzymes, glycoproteins, siRNAs, lipoproteins, aptamers, and modifications and combinations thereof. Agents can be selected from a group comprising: chemicals; small molecules; nucleic acid sequences; nucleic acid analogues; proteins; peptides; aptamers; antibodies; or fragments thereof. A nucleic acid sequence can be RNA or DNA, and can be single or double stranded, and can be selected from a group comprising; nucleic acid encoding a protein of interest, oligonucleotides, nucleic acid analogues, for example peptide—nucleic acid (PNA), pseudo-complementary PNA (pc-PNA), locked nucleic acid (LNA), modified RNA (mod-RNA), single guide RNA etc. Such nucleic acid sequences include, for example, but are not limited to, nucleic acid sequence encoding proteins, for example that act as transcriptional repressors, antisense molecules, ribozymes, small inhibitory nucleic acid sequences, for example but are not limited to RNAi, shRNAi, siRNA, micro RNAi (mRNAi), antisense oligonucleotides, CRISPR guide RNA, for example that target a CRISPR enzyme to a specific DNA target sequence etc. A protein and/or peptide or fragment thereof can be any protein of interest, for example, but are not limited to: mutated proteins; therapeutic proteins and truncated proteins, wherein the protein is normally absent or expressed at lower levels in the cell. Proteins can also be selected from a group comprising; mutated proteins, genetically engineered proteins, peptides, synthetic peptides, recombinant proteins, chimeric proteins, antibodies, midibodies, minibodies, triabodies, humanized proteins, humanized antibodies, chimeric antibodies, modified proteins and fragments thereof. Alternatively, the agent can be intracellular within the cell as a result of introduction of a nucleic acid sequence into the cell and its transcription resulting in the production of the nucleic acid and/or protein modulator of a gene within the cell. In some embodiments, the agent is any chemical, entity or moiety, including without limitation synthetic and naturally-occurring non-proteinaceous entities. In certain embodiments, the agent is a small molecule having a chemical moiety. Agents can be known to have a desired activity and/or property, or can be selected from a library of diverse compounds.

In certain embodiments, an agent may be a hormone, a cytokine, a lymphokine, a growth factor, a chemokine, a cell surface receptor ligand such as a cell surface receptor agonist or antagonist, or a mitogen.

Non-limiting examples of hormones include growth hormone (GH), adrenocorticotropic hormone (ACTH), dehydroepiandrosterone (DHEA), cortisol, epinephrine, thyroid hormone, estrogen, progesterone, testosterone, or combinations thereof.

Non-limiting examples of cytokines include lymphokines (e.g., interferon-γ, IL-2, IL-3, IL-4, IL-6, granulocyte-macrophage colony-stimulating factor (GM-CSF), interferon-γ, leukocyte migration inhibitory factors (T-LIF, B-LIF), lymphotoxin-alpha, macrophage-activating factor (MAF), macrophage migration-inhibitory factor (MIF), neuroleukin, immunologic suppressor factors, transfer factors, or combinations thereof), monokines (e.g., IL-1, TNF-alpha, interferon-α, interferon-β, colony stimulating factors, e.g., CSF2, CSF3, macrophage CSF or GM-CSF, or combinations thereof), chemokines (e.g., beta-thromboglobulin, C chemokines, CC chemokines, CXC chemokines, CX3C chemokines, macrophage inflammatory protein (MIP), or combinations thereof), interleukins (e.g., IL-1, IL-2, IL-3, IL-4, IL-5, IL-6, IL-7, IL-8, IL-9, IL-10, IL-11, IL-12, IL-13, IL-14, IL-15, IL-17, IL-18, IL-19, IL-20, IL-21, IL-22, IL-23, IL-24, IL-25, IL-26, IL-27, IL-28, IL-29, IL-30, IL-31, IL-32, IL-33, IL-34, IL-35, IL-36, or combinations thereof), and several related signalling molecules, such as tumour necrosis factor (TNF) and interferons (e.g., interferon-α, interferon-β, interferon-γ, interferon-λ, or combinations thereof).

Non-limiting examples of growth factors include those of fibroblast growth factor (FGF) family, bone morphogenic protein (BMP) family, platelet derived growth factor (PDGF) family, transforming growth factor beta (TGFbeta) family, nerve growth factor (NGF) family, epidermal growth factor (EGF) family, insulin related growth factor (IGF) family, hepatocyte growth factor (HGF) family, hematopoietic growth factors (HeGFs), platelet-derived endothelial cell growth factor (PD-ECGF), angiopoietin, vascular endothelial growth factor (VEGF) family, glucocorticoids, or combinations thereof.

Non-limiting examples of mitogens include phytohaemagglutinin (PHA), concanavalin A (conA), lipopolysaccharide (LPS), pokeweed mitogen (PWM), phorbol ester such as phorbol myristate acetate (PMA) with or without ionomycin, or combinations thereof.

Non-limiting examples of cell surface receptors the ligands of which may act as agents include Toll-like receptors (TLRs) (e.g., TLR1, TLR2, TLR3, TLR4, TLR5, TLR6, TLR7, TLR8, TLR9, TLR10, TLR11, TLR12 or TLR13), CD80, CD86, CD40, CCR7, or C-type lectin receptors.

In certain embodiments, the present invention provides for gene signature screening. The concept of signature screening was introduced by Stegmaier et al. (Gene expression-based high-throughput screening (GE-HTS) and application to leukemia differentiation. Nature Genet. 36, 257-263 (2004)), who realized that if a gene-expression signature was the proxy for a phenotype of interest, it could be used to find small molecules that effect that phenotype without knowledge of a validated drug target. The signatures of the present invention may be used to screen for drugs that induce or reduce the signature in epithelial, stromal, glia, or immune cells as described herein. The signature may be used for GE-HTS. In certain embodiments, pharmacological screens may be used to identify drugs that selectively activate gut cells. Not being bound by a theory, activation or inactivation of gut cells may have a therapeutic effect. Not being bound by a theory modulating a signature associated with disease may provide a therapeutic effect.

The Connectivity Map (cmap) is a collection of genome-wide transcriptional expression data from cultured human cells treated with bioactive small molecules and simple pattern-matching algorithms that together enable the discovery of functional connections between drugs, genes and diseases through the transitory feature of common gene-expression changes (see, Lamb et al., The Connectivity Map: Using Gene-Expression Signatures to Connect Small Molecules, Genes, and Disease. Science 29 Sep. 2006: Vol. 313, Issue 5795, pp. 1929-1935, DOI: 10.1126/science.1132939; and Lamb, J., The Connectivity Map: a new tool for biomedical research. Nature Reviews Cancer January 2007: Vol. 7, pp. 54-60). In certain embodiments, Cmap can be used to screen for small molecules capable of modulating a signature of the present invention in silico.

Particular screening applications of this invention relate to the testing of pharmaceutical compounds in drug research. The reader is referred generally to the standard textbook In vitro Methods in Pharmaceutical Research, Academic Press, 1997, and U.S. Pat. No. 5,030,015. In certain aspects of this invention, the culture of the invention is used to grow and differentiate a cachectic target cell to play the role of test cells for standard drug screening and toxicity assays. Assessment of the activity of candidate pharmaceutical compounds generally involves combining the target cell (e.g., a myocyte, an adipocyte, a cardiomyocyte or a hepatocyte) with the candidate compound, determining any change in the morphology, marker phenotype, or metabolic activity of the cells that is attributable to the candidate compound (compared with untreated cells or cells treated with an inert compound, such as vehicle), and then correlating the effect of the candidate compound with the observed change. The screening may be done because the candidate compound is designed to have a pharmacological effect on the target cell, or because a candidate compound may have unintended side effects on the target cell. Alternatively, libraries can be screened without any predetermined expectations in hopes of identifying compounds with desired effects.

Cytotoxicity can be determined in the first instance by the effect on cell viability and morphology. In certain embodiments, toxicity may be assessed by observation of vital staining techniques, ELISA assays, immunohistochemistry, and the like or by analyzing the cellular content of the culture, e.g., by total cell counts, and differential cell counts or by metabolic markers such as MTT and XTT.

Additional further uses of the culture of the invention include, but are not limited to, its use in research e.g., to elucidate mechanisms leading to the identification of novel targets for therapies, and to generate genotype-specific cells for disease modeling, including the generation of new therapies customized to different genotypes. Such customization can reduce adverse drug effects and help identify therapies appropriate to the patient's genotype.

In certain embodiments, the present invention provides method for high-throughput screening. “High-throughput screening” (HTS) refers to a process that uses a combination of modem robotics, data processing and control software, liquid handling devices, and/or sensitive detectors, to efficiently process a large amount of (e.g., thousands, hundreds of thousands, or millions of) samples in biochemical, genetic or pharmacological experiments, either in parallel or in sequence, within a reasonably short period of time (e.g., days). Preferably, the process is amenable to automation, such as robotic simultaneous handling of 96 samples, 384 samples, 1536 samples or more. A typical HTS robot tests up to 100,000 to a few hundred thousand compounds per day. The samples are often in small volumes, such as no more than 1 mL, 500 μl, 200 μl, 100 μl, 50 μl or less. Through this process, one can rapidly identify active compounds, small molecules, antibodies, proteins or polynucleotides which modulate a particular biomolecular/genetic pathway. The results of these experiments provide starting points for further drug design and for understanding the interaction or role of a particular biochemical process in biology. Thus “high-throughput screening” as used herein does not include handling large quantities of radioactive materials, slow and complicated operator-dependent screening steps, and/or prohibitively expensive reagent costs, etc

Genetic Modifying Agents

In certain embodiments, the one or more modulating agents may be a genetic modifying agent. The genetic modifying agent may comprise a CRISPR system, a zinc finger nuclease system, a TALEN, or a meganuclease.

In general, a CRISPR-Cas or CRISPR system as used in herein and in documents, such as WO 2014/093622 (PCT/US2013/074667), refers collectively to transcripts and other elements involved in the expression of or directing the activity of CRISPR-associated (“Cas”) genes, including sequences encoding a Cas gene, a tracr (trans-activating CRISPR) sequence (e.g. tracrRNA or an active partial tracrRNA), a tracr-mate sequence (encompassing a “direct repeat” and a tracrRNA-processed partial direct repeat in the context of an endogenous CRISPR system), a guide sequence (also referred to as a “spacer” in the context of an endogenous CRISPR system), or “RNA(s)” as that term is herein used (e.g., RNA(s) to guide Cas, such as Cas9, e.g. CRISPR RNA and transactivating (tracr) RNA or a single guide RNA (sgRNA) (chimeric RNA)) or other sequences and transcripts from a CRISPR locus. In general, a CRISPR system is characterized by elements that promote the formation of a CRISPR complex at the site of a target sequence (also referred to as a protospacer in the context of an endogenous CRISPR system). See, e.g, Shmakov et al. (2015) “Discovery and Functional Characterization of Diverse Class 2 CRISPR-Cas Systems”, Molecular Cell, DOI: dx.doi.org/10.1016/j.molcel.2015.10.008.

In certain embodiments, a protospacer adjacent motif (PAM) or PAM-like motif directs binding of the effector protein complex as disclosed herein to the target locus of interest. In some embodiments, the PAM may be a 5′ PAM (i.e., located upstream of the 5′ end of the protospacer). In other embodiments, the PAM may be a 3′ PAM (i.e., located downstream of the 5′ end of the protospacer). The term “PAM” may be used interchangeably with the term “PFS” or “protospacer flanking site” or “protospacer flanking sequence”.

In a preferred embodiment, the CRISPR effector protein may recognize a 3′ PAM. In certain embodiments, the CRISPR effector protein may recognize a 3′ PAM which is 5′H, wherein H is A, C or U.

In the context of formation of a CRISPR complex, “target sequence” refers to a sequence to which a guide sequence is designed to have complementarity, where hybridization between a target sequence and a guide sequence promotes the formation of a CRISPR complex. A target sequence may comprise RNA polynucleotides. The term “target RNA” refers to a RNA polynucleotide being or comprising the target sequence. In other words, the target RNA may be a RNA polynucleotide or a part of a RNA polynucleotide to which a part of the gRNA, i.e. the guide sequence, is designed to have complementarity and to which the effector function mediated by the complex comprising CRISPR effector protein and a gRNA is to be directed. In some embodiments, a target sequence is located in the nucleus or cytoplasm of a cell.

In certain example embodiments, the CRISPR effector protein may be delivered using a nucleic acid molecule encoding the CRISPR effector protein. The nucleic acid molecule encoding a CRISPR effector protein, may advantageously be a codon optimized CRISPR effector protein. An example of a codon optimized sequence, is in this instance a sequence optimized for expression in eukaryote, e.g., humans (i.e. being optimized for expression in humans), or for another eukaryote, animal or mammal as herein discussed; see, e.g., SaCas9 human codon optimized sequence in WO 2014/093622 (PCT/US2013/074667). Whilst this is preferred, it will be appreciated that other examples are possible and codon optimization for a host species other than human, or for codon optimization for specific organs is known. In some embodiments, an enzyme coding sequence encoding a CRISPR effector protein is a codon optimized for expression in particular cells, such as eukaryotic cells. The eukaryotic cells may be those of or derived from a particular organism, such as a plant or a mammal, including but not limited to human, or non-human eukaryote or animal or mammal as herein discussed, e.g., mouse, rat, rabbit, dog, livestock, or non-human mammal or primate. In some embodiments, processes for modifying the germ line genetic identity of human beings and/or processes for modifying the genetic identity of animals which are likely to cause them suffering without any substantial medical benefit to man or animal, and also animals resulting from such processes, may be excluded. In general, codon optimization refers to a process of modifying a nucleic acid sequence for enhanced expression in the host cells of interest by replacing at least one codon (e.g. about or more than about 1, 2, 3, 4, 5, 10, 15, 20, 25, 50, or more codons) of the native sequence with codons that are more frequently or most frequently used in the genes of that host cell while maintaining the native amino acid sequence. Various species exhibit particular bias for certain codons of a particular amino acid. Codon bias (differences in codon usage between organisms) often correlates with the efficiency of translation of messenger RNA (mRNA), which is in turn believed to be dependent on, among other things, the properties of the codons being translated and the availability of particular transfer RNA (tRNA) molecules. The predominance of selected tRNAs in a cell is generally a reflection of the codons used most frequently in peptide synthesis. Accordingly, genes can be tailored for optimal gene expression in a given organism based on codon optimization. Codon usage tables are readily available, for example, at the “Codon Usage Database” available at kazusa.orjp/codon/and these tables can be adapted in a number of ways. See Nakamura, Y., et al. “Codon usage tabulated from the international DNA sequence databases: status for the year 2000” Nucl. Acids Res. 28:292 (2000). Computer algorithms for codon optimizing a particular sequence for expression in a particular host cell are also available, such as Gene Forge (Aptagen; Jacobus, Pa.), are also available. In some embodiments, one or more codons (e.g. 1, 2, 3, 4, 5, 10, 15, 20, 25, 50, or more, or all codons) in a sequence encoding a Cas correspond to the most frequently used codon for a particular amino acid.

In certain embodiments, the methods as described herein may comprise providing a Cas transgenic cell in which one or more nucleic acids encoding one or more guide RNAs are provided or introduced operably connected in the cell with a regulatory element comprising a promoter of one or more gene of interest. As used herein, the term “Cas transgenic cell” refers to a cell, such as a eukaryotic cell, in which a Cas gene has been genomically integrated. The nature, type, or origin of the cell are not particularly limiting according to the present invention. Also the way the Cas transgene is introduced in the cell may vary and can be any method as is known in the art. In certain embodiments, the Cas transgenic cell is obtained by introducing the Cas transgene in an isolated cell. In certain other embodiments, the Cas transgenic cell is obtained by isolating cells from a Cas transgenic organism. By means of example, and without limitation, the Cas transgenic cell as referred to herein may be derived from a Cas transgenic eukaryote, such as a Cas knock-in eukaryote. Reference is made to WO 2014/093622 (PCT/US13/74667), incorporated herein by reference. Methods of US Patent Publication Nos. 20120017290 and 20110265198 assigned to Sangamo BioSciences, Inc. directed to targeting the Rosa locus may be modified to utilize the CRISPR Cas system of the present invention. Methods of US Patent Publication No. 20130236946 assigned to Cellectis directed to targeting the Rosa locus may also be modified to utilize the CRISPR Cas system of the present invention. By means of further example reference is made to Platt et. al. (Cell; 159(2):440-455 (2014)), describing a Cas9 knock-in mouse, which is incorporated herein by reference. The Cas transgene can further comprise a Lox-Stop-polyA-Lox(LSL) cassette thereby rendering Cas expression inducible by Cre recombinase. Alternatively, the Cas transgenic cell may be obtained by introducing the Cas transgene in an isolated cell. Delivery systems for transgenes are well known in the art. By means of example, the Cas transgene may be delivered in for instance eukaryotic cell by means of vector (e.g., AAV, adenovirus, lentivirus) and/or particle and/or nanoparticle delivery, as also described herein elsewhere.

It will be understood by the skilled person that the cell, such as the Cas transgenic cell, as referred to herein may comprise further genomic alterations besides having an integrated Cas gene or the mutations arising from the sequence specific action of Cas when complexed with RNA capable of guiding Cas to a target locus.

In certain aspects the invention involves vectors, e.g. for delivering or introducing in a cell Cas and/or RNA capable of guiding Cas to a target locus (i.e. guide RNA), but also for propagating these components (e.g. in prokaryotic cells). A used herein, a “vector” is a tool that allows or facilitates the transfer of an entity from one environment to another. It is a replicon, such as a plasmid, phage, or cosmid, into which another DNA segment may be inserted so as to bring about the replication of the inserted segment. Generally, a vector is capable of replication when associated with the proper control elements. In general, the term “vector” refers to a nucleic acid molecule capable of transporting another nucleic acid to which it has been linked. Vectors include, but are not limited to, nucleic acid molecules that are single-stranded, double-stranded, or partially double-stranded; nucleic acid molecules that comprise one or more free ends, no free ends (e.g. circular); nucleic acid molecules that comprise DNA, RNA, or both; and other varieties of polynucleotides known in the art. One type of vector is a “plasmid,” which refers to a circular double stranded DNA loop into which additional DNA segments can be inserted, such as by standard molecular cloning techniques. Another type of vector is a viral vector, wherein virally-derived DNA or RNA sequences are present in the vector for packaging into a virus (e.g. retroviruses, replication defective retroviruses, adenoviruses, replication defective adenoviruses, and adeno-associated viruses (AAVs)). Viral vectors also include polynucleotides carried by a virus for transfection into a host cell. Certain vectors are capable of autonomous replication in a host cell into which they are introduced (e.g. bacterial vectors having a bacterial origin of replication and episomal mammalian vectors). Other vectors (e.g., non-episomal mammalian vectors) are integrated into the genome of a host cell upon introduction into the host cell, and thereby are replicated along with the host genome. Moreover, certain vectors are capable of directing the expression of genes to which they are operatively-linked. Such vectors are referred to herein as “expression vectors.” Common expression vectors of utility in recombinant DNA techniques are often in the form of plasmids.

Recombinant expression vectors can comprise a nucleic acid of the invention in a form suitable for expression of the nucleic acid in a host cell, which means that the recombinant expression vectors include one or more regulatory elements, which may be selected on the basis of the host cells to be used for expression, that is operatively-linked to the nucleic acid sequence to be expressed. Within a recombinant expression vector, “operably linked” is intended to mean that the nucleotide sequence of interest is linked to the regulatory element(s) in a manner that allows for expression of the nucleotide sequence (e.g. in an in vitro transcription/translation system or in a host cell when the vector is introduced into the host cell). With regards to recombination and cloning methods, mention is made of U.S. patent application Ser. No. 10/815,730, published Sep. 2, 2004 as US 2004-0171156 A1, the contents of which are herein incorporated by reference in their entirety. Thus, the embodiments disclosed herein may also comprise transgenic cells comprising the CRISPR effector system. In certain example embodiments, the transgenic cell may function as an individual discrete volume. In other words samples comprising a masking construct may be delivered to a cell, for example in a suitable delivery vesicle and if the target is present in the delivery vesicle the CRISPR effector is activated and a detectable signal generated.

The vector(s) can include the regulatory element(s), e.g., promoter(s). The vector(s) can comprise Cas encoding sequences, and/or a single, but possibly also can comprise at least 3 or 8 or 16 or 32 or 48 or 50 guide RNA(s) (e.g., sgRNAs) encoding sequences, such as 1-2, 1-3, 1-4 1-5, 3-6, 3-7, 3-8, 3-9, 3-10, 3-8, 3-16, 3-30, 3-32, 3-48, 3-50 RNA(s) (e.g., sgRNAs). In a single vector there can be a promoter for each RNA (e.g., sgRNA), advantageously when there are up to about 16 RNA(s); and, when a single vector provides for more than 16 RNA(s), one or more promoter(s) can drive expression of more than one of the RNA(s), e.g., when there are 32 RNA(s), each promoter can drive expression of two RNA(s), and when there are 48 RNA(s), each promoter can drive expression of three RNA(s). By simple arithmetic and well established cloning protocols and the teachings in this disclosure one skilled in the art can readily practice the invention as to the RNA(s) for a suitable exemplary vector such as AAV, and a suitable promoter such as the U6 promoter. For example, the packaging limit of AAV is ˜4.7 kb. The length of a single U6-gRNA (plus restriction sites for cloning) is 361 bp. Therefore, the skilled person can readily fit about 12-16, e.g., 13 U6-gRNA cassettes in a single vector. This can be assembled by any suitable means, such as a golden gate strategy used for TALE assembly (genome-engineering.org/taleffectors/). The skilled person can also use a tandem guide strategy to increase the number of U6-gRNAs by approximately 1.5 times, e.g., to increase from 12-16, e.g., 13 to approximately 18-24, e.g., about 19 U6-gRNAs. Therefore, one skilled in the art can readily reach approximately 18-24, e.g., about 19 promoter-RNAs, e.g., U6-gRNAs in a single vector, e.g., an AAV vector. A further means for increasing the number of promoters and RNAs in a vector is to use a single promoter (e.g., U6) to express an array of RNAs separated by cleavable sequences. And an even further means for increasing the number of promoter-RNAs in a vector, is to express an array of promoter-RNAs separated by cleavable sequences in the intron of a coding sequence or gene; and, in this instance it is advantageous to use a polymerase II promoter, which can have increased expression and enable the transcription of long RNA in a tissue specific manner. (see, e.g., nar.oxfordjournals.org/content/34/7/e53.short and nature.com/mt/journal/v16/n9/abs/mt2008144a.html). In an advantageous embodiment, AAV may package U6 tandem gRNA targeting up to about 50 genes. Accordingly, from the knowledge in the art and the teachings in this disclosure the skilled person can readily make and use vector(s), e.g., a single vector, expressing multiple RNAs or guides under the control or operatively or functionally linked to one or more promoters-especially as to the numbers of RNAs or guides discussed herein, without any undue experimentation.

The guide RNA(s) encoding sequences and/or Cas encoding sequences, can be functionally or operatively linked to regulatory element(s) and hence the regulatory element(s) drive expression. The promoter(s) can be constitutive promoter(s) and/or conditional promoter(s) and/or inducible promoter(s) and/or tissue specific promoter(s). The promoter can be selected from the group consisting of RNA polymerases, pol I, pol II, pol III, T7, U6, H1, retroviral Rous sarcoma virus (RSV) LTR promoter, the cytomegalovirus (CMV) promoter, the SV40 promoter, the dihydrofolate reductase promoter, the β-actin promoter, the phosphoglycerol kinase (PGK) promoter, and the EF1α promoter. An advantageous promoter is the promoter is U6.

Additional effectors for use according to the invention can be identified by their proximity to cas1 genes, for example, though not limited to, within the region 20 kb from the start of the cas1 gene and 20 kb from the end of the cas1 gene. In certain embodiments, the effector protein comprises at least one HEPN domain and at least 500 amino acids, and wherein the C2c2 effector protein is naturally present in a prokaryotic genome within 20 kb upstream or downstream of a Cas gene or a CRISPR array. Non-limiting examples of Cas proteins include Cas1, Cas1B, Cas2, Cas3, Cas4, Cas5, Cas6, Cas7, Cas8, Cas9 (also known as Csn1 and Csx12), Cas10, Csy1, Csy2, Csy3, Cse1, Cse2, Csc1, Csc2, Csa5, Csn2, Csm2, Csm3, Csm4, Csm5, Csm6, Cmr1, Cmr3, Cmr4, Cmr5, Cmr6, Csb1, Csb2, Csb3, Csx17, Csx14, Csx10, Csx16, CsaX, Csx3, Csx1, Csx15, Csf1, Csf2, Csf3, Csf4, homologues thereof, or modified versions thereof. In certain example embodiments, the C2c2 effector protein is naturally present in a prokaryotic genome within 20 kb upstream or downstream of a Cas 1 gene. The terms “orthologue” (also referred to as “ortholog” herein) and “homologue” (also referred to as “homolog” herein) are well known in the art. By means of further guidance, a “homologue” of a protein as used herein is a protein of the same species which performs the same or a similar function as the protein it is a homologue of Homologous proteins may but need not be structurally related, or are only partially structurally related. An “orthologue” of a protein as used herein is a protein of a different species which performs the same or a similar function as the protein it is an orthologue of Orthologous proteins may but need not be structurally related, or are only partially structurally related.

Guide Molecules

The methods described herein may be used to screen inhibition of CRISPR systems employing different types of guide molecules. As used herein, the term “guide sequence” and “guide molecule” in the context of a CRISPR-Cas system, comprises any polynucleotide sequence having sufficient complementarity with a target nucleic acid sequence to hybridize with the target nucleic acid sequence and direct sequence-specific binding of a nucleic acid-targeting complex to the target nucleic acid sequence. The guide sequences made using the methods disclosed herein may be a full-length guide sequence, a truncated guide sequence, a full-length sgRNA sequence, a truncated sgRNA sequence, or an E+F sgRNA sequence. In some embodiments, the degree of complementarity of the guide sequence to a given target sequence, when optimally aligned using a suitable alignment algorithm, is about or more than about 50%, 60%, 75%, 80%, 85%, 90%, 95%, 97.5%, 99%, or more. In certain example embodiments, the guide molecule comprises a guide sequence that may be designed to have at least one mismatch with the target sequence, such that a RNA duplex formed between the guide sequence and the target sequence. Accordingly, the degree of complementarity is preferably less than 99%. For instance, where the guide sequence consists of 24 nucleotides, the degree of complementarity is more particularly about 96% or less. In particular embodiments, the guide sequence is designed to have a stretch of two or more adjacent mismatching nucleotides, such that the degree of complementarity over the entire guide sequence is further reduced. For instance, where the guide sequence consists of 24 nucleotides, the degree of complementarity is more particularly about 96% or less, more particularly, about 92% or less, more particularly about 88% or less, more particularly about 84% or less, more particularly about 80% or less, more particularly about 76% or less, more particularly about 72% or less, depending on whether the stretch of two or more mismatching nucleotides encompasses 2, 3, 4, 5, 6 or 7 nucleotides, etc. In some embodiments, aside from the stretch of one or more mismatching nucleotides, the degree of complementarity, when optimally aligned using a suitable alignment algorithm, is about or more than about 50%, 60%, 75%, 80%, 85%, 90%, 95%, 97.5%, 99%, or more. Optimal alignment may be determined with the use of any suitable algorithm for aligning sequences, non-limiting example of which include the Smith-Waterman algorithm, the Needleman-Wunsch algorithm, algorithms based on the Burrows-Wheeler Transform (e.g., the Burrows Wheeler Aligner), ClustalW, Clustal X, BLAT, Novoalign (Novocraft Technologies; available at www.novocraft.com), ELAND (Illumina, San Diego, Calif.), SOAP (available at soap.genomics.org.cn), and Maq (available at maq.sourceforge.net). The ability of a guide sequence (within a nucleic acid-targeting guide RNA) to direct sequence-specific binding of a nucleic acid-targeting complex to a target nucleic acid sequence may be assessed by any suitable assay. For example, the components of a nucleic acid-targeting CRISPR system sufficient to form a nucleic acid-targeting complex, including the guide sequence to be tested, may be provided to a host cell having the corresponding target nucleic acid sequence, such as by transfection with vectors encoding the components of the nucleic acid-targeting complex, followed by an assessment of preferential targeting (e.g., cleavage) within the target nucleic acid sequence, such as by Surveyor assay as described herein. Similarly, cleavage of a target nucleic acid sequence (or a sequence in the vicinity thereof) may be evaluated in a test tube by providing the target nucleic acid sequence, components of a nucleic acid-targeting complex, including the guide sequence to be tested and a control guide sequence different from the test guide sequence, and comparing binding or rate of cleavage at or in the vicinity of the target sequence between the test and control guide sequence reactions. Other assays are possible, and will occur to those skilled in the art. A guide sequence, and hence a nucleic acid-targeting guide RNA may be selected to target any target nucleic acid sequence.

In certain embodiments, the guide sequence or spacer length of the guide molecules is from 15 to 50 nt. In certain embodiments, the spacer length of the guide RNA is at least 15 nucleotides. In certain embodiments, the spacer length is from 15 to 17 nt, e.g., 15, 16, or 17 nt, from 17 to 20 nt, e.g., 17, 18, 19, or 20 nt, from 20 to 24 nt, e.g., 20, 21, 22, 23, or 24 nt, from 23 to 25 nt, e.g., 23, 24, or 25 nt, from 24 to 27 nt, e.g., 24, 25, 26, or 27 nt, from 27-30 nt, e.g., 27, 28, 29, or 30 nt, from 30-35 nt, e.g., 30, 31, 32, 33, 34, or 35 nt, or 35 nt or longer. In certain example embodiment, the guide sequence is 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 31, 32, 33, 34, 35, 36, 37, 38, 3940, 41, 42, 43, 44, 45, 46, 4748, 49, 50, 51, 52, 53, 54, 55, 56, 57, 58, 59, 60, 61, 62, 63, 64, 65, 66, 67, 68, 69, 70, 71, 72, 73, 74, 75, 76, 77, 78, 79, 80, 81, 82, 83, 84, 85, 86, 87, 88, 89, 90, 91, 92, 93, 94, 95, 96, 97, 98, 99, or 100 nt.

In some embodiments, the guide sequence is an RNA sequence of between 10 to 50 nt in length, but more particularly of about 20-30 nt advantageously about 20 nt, 23-25 nt or 24 nt. The guide sequence is selected so as to ensure that it hybridizes to the target sequence. This is described more in detail below. Selection can encompass further steps which increase efficacy and specificity.

In some embodiments, the guide sequence has a canonical length (e.g., about 15-30 nt) is used to hybridize with the target RNA or DNA. In some embodiments, a guide molecule is longer than the canonical length (e.g., >30 nt) is used to hybridize with the target RNA or DNA, such that a region of the guide sequence hybridizes with a region of the RNA or DNA strand outside of the Cas-guide target complex. This can be of interest where additional modifications, such deamination of nucleotides is of interest. In alternative embodiments, it is of interest to maintain the limitation of the canonical guide sequence length.

In some embodiments, the sequence of the guide molecule (direct repeat and/or spacer) is selected to reduce the degree secondary structure within the guide molecule. In some embodiments, about or less than about 75%, 50%, 40%, 30%, 25%, 20%, 15%, 10%, 5%, 1%, or fewer of the nucleotides of the nucleic acid-targeting guide RNA participate in self-complementary base pairing when optimally folded. Optimal folding may be determined by any suitable polynucleotide folding algorithm. Some programs are based on calculating the minimal Gibbs free energy. An example of one such algorithm is mFold, as described by Zuker and Stiegler (Nucleic Acids Res. 9 (1981), 133-148). Another example folding algorithm is the online webserver RNAfold, developed at Institute for Theoretical Chemistry at the University of Vienna, using the centroid structure prediction algorithm (see e.g., A. R. Gruber et al., 2008, Cell 106(1): 23-24; and P A Carr and G M Church, 2009, Nature Biotechnology 27(12): 1151-62).

In some embodiments, it is of interest to reduce the susceptibility of the guide molecule to RNA cleavage, such as to cleavage by Cas13. Accordingly, in particular embodiments, the guide molecule is adjusted to avoide cleavage by Cas13 or other RNA-cleaving enzymes.

In certain embodiments, the guide molecule comprises non-naturally occurring nucleic acids and/or non-naturally occurring nucleotides and/or nucleotide analogs, and/or chemically modifications. Preferably, these non-naturally occurring nucleic acids and non-naturally occurring nucleotides are located outside the guide sequence. Non-naturally occurring nucleic acids can include, for example, mixtures of naturally and non-naturally occurring nucleotides. Non-naturally occurring nucleotides and/or nucleotide analogs may be modified at the ribose, phosphate, and/or base moiety. In an embodiment of the invention, a guide nucleic acid comprises ribonucleotides and non-ribonucleotides. In one such embodiment, a guide comprises one or more ribonucleotides and one or more deoxyribonucleotides. In an embodiment of the invention, the guide comprises one or more non-naturally occurring nucleotide or nucleotide analog such as a nucleotide with phosphorothioate linkage, a locked nucleic acid (LNA) nucleotides comprising a methylene bridge between the 2′ and 4′ carbons of the ribose ring, or bridged nucleic acids (BNA). Other examples of modified nucleotides include 2′-O-methyl analogs, 2′-deoxy analogs, or 2′-fluoro analogs. Further examples of modified bases include, but are not limited to, 2-aminopurine, 5-bromo-uridine, pseudouridine, inosine, 7-methylguanosine. Examples of guide RNA chemical modifications include, without limitation, incorporation of 2′-O-methyl (M), 2′-O-methyl 3′phosphorothioate (MS), S-constrained ethyl(cEt), or 2′-O-methyl 3′thioPACE (MSP) at one or more terminal nucleotides. Such chemically modified guides can comprise increased stability and increased activity as compared to unmodified guides, though on-target vs. off-target specificity is not predictable. (See, Hendel, 2015, Nat Biotechnol. 33(9):985-9, doi: 10.1038/nbt.3290, published online 29 Jun. 2015 Ragdarm et al., 0215, PNAS, E7110-E7111; Allerson et al., J. Med. Chem. 2005, 48:901-904; Bramsen et al., Front. Genet., 2012, 3:154; Deng et al., PNAS, 2015, 112:11870-11875; Sharma et al., MedChemComm., 2014, 5:1454-1471; Hendel et al., Nat. Biotechnol. (2015) 33(9): 985-989; Li et al., Nature Biomedical Engineering, 2017, 1, 0066 DOI:10.1038/s41551-017-0066). In some embodiments, the 5′ and/or 3′ end of a guide RNA is modified by a variety of functional moieties including fluorescent dyes, polyethylene glycol, cholesterol, proteins, or detection tags. (See Kelly et al., 2016, J. Biotech. 233:74-83). In certain embodiments, a guide comprises ribonucleotides in a region that binds to a target RNA and one or more deoxyribonucletides and/or nucleotide analogs in a region that binds to Cas13. In an embodiment of the invention, deoxyribonucleotides and/or nucleotide analogs are incorporated in engineered guide structures, such as, without limitation, stem-loop regions, and the seed region. For Cas13 guide, in certain embodiments, the modification is not in the 5′-handle of the stem-loop regions. Chemical modification in the 5′-handle of the stem-loop region of a guide may abolish its function (see Li, et al., Nature Biomedical Engineering, 2017, 1:0066). In certain embodiments, at least 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, 30, 35, 40, 45, 50, or 75 nucleotides of a guide is chemically modified. In some embodiments, 3-5 nucleotides at either the 3′ or the 5′ end of a guide is chemically modified. In some embodiments, only minor modifications are introduced in the seed region, such as 2′-F modifications. In some embodiments, 2′-F modification is introduced at the 3′ end of a guide. In certain embodiments, three to five nucleotides at the 5′ and/or the 3′ end of the guide are chemicially modified with 2′-O-methyl (M), 2′-O-methyl 3′ phosphorothioate (MS), S-constrained ethyl(cEt), or 2′-O-methyl 3′ thioPACE (MSP). Such modification can enhance genome editing efficiency (see Hendel et al., Nat. Biotechnol. (2015) 33(9): 985-989). In certain embodiments, all of the phosphodiester bonds of a guide are substituted with phosphorothioates (PS) for enhancing levels of gene disruption. In certain embodiments, more than five nucleotides at the 5′ and/or the 3′ end of the guide are chemicially modified with 2′-O-Me, 2′-F or S-constrained ethyl(cEt). Such chemically modified guide can mediate enhanced levels of gene disruption (see Ragdarm et al., 0215, PNAS, E7110-E7111). In an embodiment of the invention, a guide is modified to comprise a chemical moiety at its 3′ and/or 5′ end. Such moieties include, but are not limited to amine, azide, alkyne, thio, dibenzocyclooctyne (DBCO), or Rhodamine. In certain embodiment, the chemical moiety is conjugated to the guide by a linker, such as an alkyl chain. In certain embodiments, the chemical moiety of the modified guide can be used to attach the guide to another molecule, such as DNA, RNA, protein, or nanoparticles. Such chemically modified guide can be used to identify or enrich cells generically edited by a CRISPR system (see Lee et al., eLife, 2017, 6:e25312, DOI:10.7554).

In some embodiments, the modification to the guide is a chemical modification, an insertion, a deletion or a split. In some embodiments, the chemical modification includes, but is not limited to, incorporation of 2′-O-methyl (M) analogs, 2′-deoxy analogs, 2-thiouridine analogs, N6-methyladenosine analogs, 2′-fluoro analogs, 2-aminopurine, 5-bromo-uridine, pseudouridine (Ψ), N1-methylpseudouridine (melΨ), 5-methoxyuridine(5moU), inosine, 7-methylguanosine, 2′-O-methyl 3′phosphorothioate (MS), S-constrained ethyl(cEt), phosphorothioate (PS), or 2′-O-methyl 3′thioPACE (MSP). In some embodiments, the guide comprises one or more of phosphorothioate modifications. In certain embodiments, at least 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11, 12, 13, 14, 15, 16, 17, 18, 19, 20, or 25 nucleotides of the guide are chemically modified. In certain embodiments, one or more nucleotides in the seed region are chemically modified. In certain embodiments, one or more nucleotides in the 3′-terminus are chemically modified. In certain embodiments, none of the nucleotides in the 5′-handle is chemically modified. In some embodiments, the chemical modification in the seed region is a minor modification, such as incorporation of a 2′-fluoro analog. In a specific embodiment, one nucleotide of the seed region is replaced with a 2′-fluoro analog. In some embodiments, 5 to 10 nucleotides in the 3′-terminus are chemically modified. Such chemical modifications at the 3′-terminus of the Cas13 CrRNA may improve Cas13 activity. In a specific embodiment, 1, 2, 3, 4, 5, 6, 7, 8, 9 or 10 nucleotides in the 3′-terminus are replaced with 2′-fluoro analogues. In a specific embodiment, 1, 2, 3, 4, 5, 6, 7, 8, 9 or 10 nucleotides in the 3′-terminus are replaced with 2′-O-methyl (M) analogs.

In some embodiments, the loop of the 5′-handle of the guide is modified. In some embodiments, the loop of the 5′-handle of the guide is modified to have a deletion, an insertion, a split, or chemical modifications. In certain embodiments, the modified loop comprises 3, 4, or 5 nucleotides. In certain embodiments, the loop comprises the sequence of UCUU, UUUU, UAUU, or UGUU.

In some embodiments, the guide molecule forms a stemloop with a separate non-covalently linked sequence, which can be DNA or RNA. In particular embodiments, the sequences forming the guide are first synthesized using the standard phosphoramidite synthetic protocol (Herdewijn, P., ed., Methods in Molecular Biology Col 288, Oligonucleotide Synthesis: Methods and Applications, Humana Press, New Jersey (2012)). In some embodiments, these sequences can be functionalized to contain an appropriate functional group for ligation using the standard protocol known in the art (Hermanson, G. T., Bioconjugate Techniques, Academic Press (2013)). Examples of functional groups include, but are not limited to, hydroxyl, amine, carboxylic acid, carboxylic acid halide, carboxylic acid active ester, aldehyde, carbonyl, chlorocarbonyl, imidazolylcarbonyl, hydrozide, semicarbazide, thio semicarbazide, thiol, maleimide, haloalkyl, sufonyl, ally, propargyl, diene, alkyne, and azide. Once this sequence is functionalized, a covalent chemical bond or linkage can be formed between this sequence and the direct repeat sequence. Examples of chemical bonds include, but are not limited to, those based on carbamates, ethers, esters, amides, imines, amidines, aminotrizines, hydrozone, disulfides, thioethers, thioesters, phosphorothioates, phosphorodithioates, sulfonamides, sulfonates, fulfones, sulfoxides, ureas, thioureas, hydrazide, oxime, triazole, photolabile linkages, C—C bond forming groups such as Diels-Alder cyclo-addition pairs or ring-closing metathesis pairs, and Michael reaction pairs.

In some embodiments, these stem-loop forming sequences can be chemically synthesized. In some embodiments, the chemical synthesis uses automated, solid-phase oligonucleotide synthesis machines with 2′-acetoxyethyl orthoester (2′-ACE) (Scaringe et al., J. Am. Chem. Soc. (1998) 120: 11820-11821; Scaringe, Methods Enzymol. (2000) 317: 3-18) or 2′-thionocarbamate (2′-TC) chemistry (Dellinger et al., J. Am. Chem. Soc. (2011) 133: 11540-11546; Hendel et al., Nat. Biotechnol. (2015) 33:985-989).

In certain embodiments, the guide molecule comprises (1) a guide sequence capable of hybridizing to a target locus and (2) a tracr mate or direct repeat sequence whereby the direct repeat sequence is located upstream (i.e., 5′) from the guide sequence. In a particular embodiment the seed sequence (i.e. the sequence essential critical for recognition and/or hybridization to the sequence at the target locus) of th guide sequence is approximately within the first 10 nucleotides of the guide sequence.

In a particular embodiment the guide molecule comprises a guide sequence linked to a direct repeat sequence, wherein the direct repeat sequence comprises one or more stem loops or optimized secondary structures. In particular embodiments, the direct repeat has a minimum length of 16 nts and a single stem loop. In further embodiments the direct repeat has a length longer than 16 nts, preferably more than 17 nts, and has more than one stem loops or optimized secondary structures. In particular embodiments the guide molecule comprises or consists of the guide sequence linked to all or part of the natural direct repeat sequence. A typical Type V or Type VI CRISPR-cas guide molecule comprises (in 3′ to 5′ direction or in 5′ to 3′ direction): a guide sequence a first complimentary stretch (the “repeat”), a loop (which is typically 4 or 5 nucleotides long), a second complimentary stretch (the “anti-repeat” being complimentary to the repeat), and a poly A (often poly U in RNA) tail (terminator). In certain embodiments, the direct repeat sequence retains its natural architecture and forms a single stem loop. In particular embodiments, certain aspects of the guide architecture can be modified, for example by addition, subtraction, or substitution of features, whereas certain other aspects of guide architecture are maintained. Preferred locations for engineered guide molecule modifications, including but not limited to insertions, deletions, and substitutions include guide termini and regions of the guide molecule that are exposed when complexed with the CRISPR-Cas protein and/or target, for example the stemloop of the direct repeat sequence.

In particular embodiments, the stem comprises at least about 4 bp comprising complementary X and Y sequences, although stems of more, e.g., 5, 6, 7, 8, 9, 10, 11 or 12 or fewer, e.g., 3, 2, base pairs are also contemplated. Thus, for example X2-10 and Y2-10 (wherein X and Y represent any complementary set of nucleotides) may be contemplated. In one aspect, the stem made of the X and Y nucleotides, together with the loop will form a complete hairpin in the overall secondary structure; and, this may be advantageous and the amount of base pairs can be any amount that forms a complete hairpin. In one aspect, any complementary X:Y basepairing sequence (e.g., as to length) is tolerated, so long as the secondary structure of the entire guide molecule is preserved. In one aspect, the loop that connects the stem made of X:Y basepairs can be any sequence of the same length (e.g., 4 or 5 nucleotides) or longer that does not interrupt the overall secondary structure of the guide molecule. In one aspect, the stemloop can further comprise, e.g. an MS2 aptamer. In one aspect, the stem comprises about 5-7 bp comprising complementary X and Y sequences, although stems of more or fewer basepairs are also contemplated. In one aspect, non-Watson Crick basepairing is contemplated, where such pairing otherwise generally preserves the architecture of the stemloop at that position.

In particular embodiments the natural hairpin or stemloop structure of the guide molecule is extended or replaced by an extended stemloop. It has been demonstrated that extension of the stem can enhance the assembly of the guide molecule with the CRISPR-Cas proten (Chen et al. Cell. (2013); 155(7): 1479-1491). In particular embodiments the stem of the stemloop is extended by at least 1, 2, 3, 4, 5 or more complementary basepairs (i.e. corresponding to the addition of 2, 4, 6, 8, 10 or more nucleotides in the guide molecule). In particular embodiments these are located at the end of the stem, adjacent to the loop of the stemloop.

In particular embodiments, the susceptibility of the guide molecule to RNAses or to decreased expression can be reduced by slight modifications of the sequence of the guide molecule which do not affect its function. For instance, in particular embodiments, premature termination of transcription, such as premature transcription of U6 Pol-III, can be removed by modifying a putative Pol-III terminator (4 consecutive U's) in the guide molecules sequence. Where such sequence modification is required in the stemloop of the guide molecule, it is preferably ensured by a basepair flip.

In a particular embodiment, the direct repeat may be modified to comprise one or more protein-binding RNA aptamers. In a particular embodiment, one or more aptamers may be included such as part of optimized secondary structure. Such aptamers may be capable of binding a bacteriophage coat protein as detailed further herein.

In some embodiments, the guide molecule forms a duplex with a target RNA comprising at least one target cytosine residue to be edited. Upon hybridization of the guide RNA molecule to the target RNA, the cytidine deaminase binds to the single strand RNA in the duplex made accessible by the mismatch in the guide sequence and catalyzes deamination of one or more target cytosine residues comprised within the stretch of mismatching nucleotides.

A guide sequence, and hence a nucleic acid-targeting guide RNA may be selected to target any target nucleic acid sequence. The target sequence may be mRNA.

In certain embodiments, the target sequence should be associated with a PAM (protospacer adjacent motif) or PFS (protospacer flanking sequence or site); that is, a short sequence recognized by the CRISPR complex. Depending on the nature of the CRISPR-Cas protein, the target sequence should be selected such that its complementary sequence in the DNA duplex (also referred to herein as the non-target sequence) is upstream or downstream of the PAM. In the embodiments of the present invention where the CRISPR-Cas protein is a Cas13 protein, the compelementary sequence of the target sequence is downstream or 3′ of the PAM or upstream or 5′ of the PAM. The precise sequence and length requirements for the PAM differ depending on the Cas13 protein used, but PAMs are typically 2-5 base pair sequences adjacent the protospacer (that is, the target sequence). Examples of the natural PAM sequences for different Cas13 orthologues are provided herein below and the skilled person will be able to identify further PAM sequences for use with a given Cas13 protein.

Further, engineering of the PAM Interacting (PI) domain may allow programing of PAM specificity, improve target site recognition fidelity, and increase the versatility of the CRISPR-Cas protein, for example as described for Cas9 in Kleinstiver B P et al. Engineered CRISPR-Cas9 nucleases with altered PAM specificities. Nature. 2015 Jul. 23; 523(7561):481-5. doi: 10.1038/nature14592. As further detailed herein, the skilled person will understand that Cas13 proteins may be modified analogously.

In particular embodiment, the guide is an escorted guide. By “escorted” is meant that the CRISPR-Cas system or complex or guide is delivered to a selected time or place within a cell, so that activity of the CRISPR-Cas system or complex or guide is spatially or temporally controlled. For example, the activity and destination of the 3 CRISPR-Cas system or complex or guide may be controlled by an escort RNA aptamer sequence that has binding affinity for an aptamer ligand, such as a cell surface protein or other localized cellular component. Alternatively, the escort aptamer may for example be responsive to an aptamer effector on or in the cell, such as a transient effector, such as an external energy source that is applied to the cell at a particular time.

The escorted CRISPR-Cas systems or complexes have a guide molecule with a functional structure designed to improve guide molecule structure, architecture, stability, genetic expression, or any combination thereof. Such a structure can include an aptamer.

Aptamers are biomolecules that can be designed or selected to bind tightly to other ligands, for example using a technique called systematic evolution of ligands by exponential enrichment (SELEX; Tuerk C, Gold L: “Systematic evolution of ligands by exponential enrichment: RNA ligands to bacteriophage T4 DNA polymerase.” Science 1990, 249:505-510). Nucleic acid aptamers can for example be selected from pools of random-sequence oligonucleotides, with high binding affinities and specificities for a wide range of biomedically relevant targets, suggesting a wide range of therapeutic utilities for aptamers (Keefe, Anthony D., Supriya Pai, and Andrew Ellington. “Aptamers as therapeutics.” Nature Reviews Drug Discovery 9.7 (2010): 537-550). These characteristics also suggest a wide range of uses for aptamers as drug delivery vehicles (Levy-Nissenbaum, Etgar, et al. “Nanotechnology and aptamers: applications in drug delivery.” Trends in biotechnology 26.8 (2008): 442-449; and, Hicke B J, Stephens A W. “Escort aptamers: a delivery service for diagnosis and therapy.” J Clin Invest 2000, 106:923-928.). Aptamers may also be constructed that function as molecular switches, responding to a que by changing properties, such as RNA aptamers that bind fluorophores to mimic the activity of green flourescent protein (Paige, Jeremy S., Karen Y. Wu, and Samie R. Jaffrey. “RNA mimics of green fluorescent protein.” Science 333.6042 (2011): 642-646). It has also been suggested that aptamers may be used as components of targeted siRNA therapeutic delivery systems, for example targeting cell surface proteins (Zhou, Jiehua, and John J. Rossi. “Aptamer-targeted cell-specific RNA interference.” Silence 1.1 (2010): 4).

Accordingly, in particular embodiments, the guide molecule is modified, e.g., by one or more aptamer(s) designed to improve guide molecule delivery, including delivery across the cellular membrane, to intracellular compartments, or into the nucleus. Such a structure can include, either in addition to the one or more aptamer(s) or without such one or more aptamer(s), moiety(ies) so as to render the guide molecule deliverable, inducible or responsive to a selected effector. The invention accordingly comprehends an guide molecule that responds to normal or pathological physiological conditions, including without limitation pH, hypoxia, O₂ concentration, temperature, protein concentration, enzymatic concentration, lipid structure, light exposure, mechanical disruption (e.g. ultrasound waves), magnetic fields, electric fields, or electromagnetic radiation.

Light responsiveness of an inducible system may be achieved via the activation and binding of cryptochrome-2 and CIB1. Blue light stimulation induces an activating conformational change in cryptochrome-2, resulting in recruitment of its binding partner CIB1. This binding is fast and reversible, achieving saturation in <15 see following pulsed stimulation and returning to baseline <15 min after the end of stimulation. These rapid binding kinetics result in a system temporally bound only by the speed of transcription/translation and transcript/protein degradation, rather than uptake and clearance of inducing agents. Crytochrome-2 activation is also highly sensitive, allowing for the use of low light intensity stimulation and mitigating the risks of phototoxicity. Further, in a context such as the intact mammalian brain, variable light intensity may be used to control the size of a stimulated region, allowing for greater precision than vector delivery alone may offer.

The invention contemplates energy sources such as electromagnetic radiation, sound energy or thermal energy to induce the guide. Advantageously, the electromagnetic radiation is a component of visible light. In a preferred embodiment, the light is a blue light with a wavelength of about 450 to about 495 nm. In an especially preferred embodiment, the wavelength is about 488 nm. In another preferred embodiment, the light stimulation is via pulses. The light power may range from about 0-9 mW/cm². In a preferred embodiment, a stimulation paradigm of as low as 0.25 sec every 15 sec should result in maximal activation.

The chemical or energy sensitive guide may undergo a conformational change upon induction by the binding of a chemical source or by the energy allowing it act as a guide and have the Cas13 CRISPR-Cas system or complex function. The invention can involve applying the chemical source or energy so as to have the guide function and the Cas13 CRISPR-Cas system or complex function; and optionally further determining that the expression of the genomic locus is altered.

There are several different designs of this chemical inducible system: 1. ABI-PYL based system inducible by Abscisic Acid (ABA) (see, e.g., stke.sciencemag.org/cgi/content/abstract/sigtrans; 4/164/rs2), 2. FKBP-FRB based system inducible by rapamycin (or related chemicals based on rapamycin) (see, e.g., www.nature.com/nmeth/joumal/v2/n6/full/nmeth763.html), 3. GID1-GAI based system inducible by Gibberellin (GA) (see, e.g., www.nature.com/nchembio/joumal/v8/n5/full/nchembio.922.html).

A chemical inducible system can be an estrogen receptor (ER) based system inducible by 4-hydroxytamoxifen (40HT) (see, e.g., www.pnas.org/content/104/3/1027.abstract). A mutated ligand-binding domain of the estrogen receptor called ERT2 translocates into the nucleus of cells upon binding of 4-hydroxytamoxifen. In further embodiments of the invention any naturally occurring or engineered derivative of any nuclear receptor, thyroid hormone receptor, retinoic acid receptor, estrogren receptor, estrogen-related receptor, glucocorticoid receptor, progesterone receptor, androgen receptor may be used in inducible systems analogous to the ER based inducible system.

Another inducible system is based on the design using Transient receptor potential (TRP) ion channel based system inducible by energy, heat or radio-wave (see, e.g., www.sciencemag.org/content/336/6081/604). These TRP family proteins respond to different stimuli, including light and heat. When this protein is activated by light or heat, the ion channel will open and allow the entering of ions such as calcium into the plasma membrane. This influx of ions will bind to intracellular ion interacting partners linked to a polypeptide including the guide and the other components of the Cas13 CRISPR-Cas complex or system, and the binding will induce the change of sub-cellular localization of the polypeptide, leading to the entire polypeptide entering the nucleus of cells. Once inside the nucleus, the guide protein and the other components of the Cas13 CRISPR-Cas complex will be active and modulating target gene expression in cells.

While light activation may be an advantageous embodiment, sometimes it may be disadvantageous especially for in vivo applications in which the light may not penetrate the skin or other organs. In this instance, other methods of energy activation are contemplated, in particular, electric field energy and/or ultrasound which have a similar effect.

Electric field energy is preferably administered substantially as described in the art, using one or more electric pulses of from about 1 Volt/cm to about 10 kVolts/cm under in vivo conditions. Instead of or in addition to the pulses, the electric field may be delivered in a continuous manner. The electric pulse may be applied for between 1 μs and 500 milliseconds, preferably between 1 μs and 100 milliseconds. The electric field may be applied continuously or in a pulsed manner for 5 about minutes.

As used herein, ‘electric field energy’ is the electrical energy to which a cell is exposed. Preferably the electric field has a strength of from about 1 Volt/cm to about 10 kVolts/cm or more under in vivo conditions (see WO97/49450).

As used herein, the term “electric field” includes one or more pulses at variable capacitance and voltage and including exponential and/or square wave and/or modulated wave and/or modulated square wave forms. References to electric fields and electricity should be taken to include reference the presence of an electric potential difference in the environment of a cell. Such an environment may be set up by way of static electricity, alternating current (AC), direct current (DC), etc, as known in the art. The electric field may be uniform, non-uniform or otherwise, and may vary in strength and/or direction in a time dependent manner.

Single or multiple applications of electric field, as well as single or multiple applications of ultrasound are also possible, in any order and in any combination. The ultrasound and/or the electric field may be delivered as single or multiple continuous applications, or as pulses (pulsatile delivery).

Electroporation has been used in both in vitro and in vivo procedures to introduce foreign material into living cells. With in vitro applications, a sample of live cells is first mixed with the agent of interest and placed between electrodes such as parallel plates. Then, the electrodes apply an electrical field to the cell/implant mixture. Examples of systems that perform in vitro electroporation include the Electro Cell Manipulator ECM600 product, and the Electro Square Porator T820, both made by the BTX Division of Genetronics, Inc (see U.S. Pat. No. 5,869,326).

The known electroporation techniques (both in vitro and in vivo) function by applying a brief high voltage pulse to electrodes positioned around the treatment region. The electric field generated between the electrodes causes the cell membranes to temporarily become porous, whereupon molecules of the agent of interest enter the cells. In known electroporation applications, this electric field comprises a single square wave pulse on the order of 1000 V/cm, of about 100.mu.s duration. Such a pulse may be generated, for example, in known applications of the Electro Square Porator T820.

Preferably, the electric field has a strength of from about 1 V/cm to about 10 kV/cm under in vitro conditions. Thus, the electric field may have a strength of 1 V/cm, 2 V/cm, 3 V/cm, 4 V/cm, 5 V/cm, 6 V/cm, 7 V/cm, 8 V/cm, 9 V/cm, 10 V/cm, 20 V/cm, 50 V/cm, 100 V/cm, 200 V/cm, 300 V/cm, 400 V/cm, 500 V/cm, 600 V/cm, 700 V/cm, 800 V/cm, 900 V/cm, 1 kV/cm, 2 kV/cm, 5 kV/cm, 10 kV/cm, 20 kV/cm, 50 kV/cm or more. More preferably from about 0.5 kV/cm to about 4.0 kV/cm under in vitro conditions. Preferably the electric field has a strength of from about 1 V/cm to about 10 kV/cm under in vivo conditions. However, the electric field strengths may be lowered where the number of pulses delivered to the target site are increased. Thus, pulsatile delivery of electric fields at lower field strengths is envisaged.

Preferably the application of the electric field is in the form of multiple pulses such as double pulses of the same strength and capacitance or sequential pulses of varying strength and/or capacitance. As used herein, the term “pulse” includes one or more electric pulses at variable capacitance and voltage and including exponential and/or square wave and/or modulated wave/square wave forms.

Preferably the electric pulse is delivered as a waveform selected from an exponential wave form, a square wave form, a modulated wave form and a modulated square wave form.

A preferred embodiment employs direct current at low voltage. Thus, Applicants disclose the use of an electric field which is applied to the cell, tissue or tissue mass at a field strength of between 1V/cm and 20V/cm, for a period of 100 milliseconds or more, preferably 15 minutes or more.

Ultrasound is advantageously administered at a power level of from about 0.05 W/cm2 to about 100 W/cm2. Diagnostic or therapeutic ultrasound may be used, or combinations thereof.

As used herein, the term “ultrasound” refers to a form of energy which consists of mechanical vibrations the frequencies of which are so high they are above the range of human hearing. Lower frequency limit of the ultrasonic spectrum may generally be taken as about 20 kHz. Most diagnostic applications of ultrasound employ frequencies in the range 1 and 15 MHz′ (From Ultrasonics in Clinical Diagnosis, P. N. T. Wells, ed., 2nd. Edition, Publ. Churchill Livingstone [Edinburgh, London & NY, 1977]).

Ultrasound has been used in both diagnostic and therapeutic applications. When used as a diagnostic tool (“diagnostic ultrasound”), ultrasound is typically used in an energy density range of up to about 100 mW/cm2 (FDA recommendation), although energy densities of up to 750 mW/cm2 have been used. In physiotherapy, ultrasound is typically used as an energy source in a range up to about 3 to 4 W/cm2 (WHO recommendation). In other therapeutic applications, higher intensities of ultrasound may be employed, for example, HIFU at 100 W/cm up to 1 kW/cm2 (or even higher) for short periods of time. The term “ultrasound” as used in this specification is intended to encompass diagnostic, therapeutic and focused ultrasound.

Focused ultrasound (FUS) allows thermal energy to be delivered without an invasive probe (see Morocz et al 1998 Journal of Magnetic Resonance Imaging Vol. 8, No. 1, pp. 136-142. Another form of focused ultrasound is high intensity focused ultrasound (HIFU) which is reviewed by Moussatov et al in Ultrasonics (1998) Vol. 36, No. 8, pp. 893-900 and TranHuuHue et al in Acustica (1997) Vol. 83, No. 6, pp. 1103-1106.

Preferably, a combination of diagnostic ultrasound and a therapeutic ultrasound is employed. This combination is not intended to be limiting, however, and the skilled reader will appreciate that any variety of combinations of ultrasound may be used. Additionally, the energy density, frequency of ultrasound, and period of exposure may be varied.

Preferably the exposure to an ultrasound energy source is at a power density of from about 0.05 to about 100 Wcm-2. Even more preferably, the exposure to an ultrasound energy source is at a power density of from about 1 to about 15 Wcm-2.

Preferably the exposure to an ultrasound energy source is at a frequency of from about 0.015 to about 10.0 MHz. More preferably the exposure to an ultrasound energy source is at a frequency of from about 0.02 to about 5.0 MHz or about 6.0 MHz. Most preferably, the ultrasound is applied at a frequency of 3 MHz.

Preferably the exposure is for periods of from about 10 milliseconds to about 60 minutes. Preferably the exposure is for periods of from about 1 second to about 5 minutes. More preferably, the ultrasound is applied for about 2 minutes. Depending on the particular target cell to be disrupted, however, the exposure may be for a longer duration, for example, for 15 minutes.

Advantageously, the target tissue is exposed to an ultrasound energy source at an acoustic power density of from about 0.05 Wcm-2 to about 10 Wcm-2 with a frequency ranging from about 0.015 to about 10 MHz (see WO 98/52609). However, alternatives are also possible, for example, exposure to an ultrasound energy source at an acoustic power density of above 100 Wcm-2, but for reduced periods of time, for example, 1000 Wcm-2 for periods in the millisecond range or less.

Preferably the application of the ultrasound is in the form of multiple pulses; thus, both continuous wave and pulsed wave (pulsatile delivery of ultrasound) may be employed in any combination. For example, continuous wave ultrasound may be applied, followed by pulsed wave ultrasound, or vice versa. This may be repeated any number of times, in any order and combination. The pulsed wave ultrasound may be applied against a background of continuous wave ultrasound, and any number of pulses may be used in any number of groups.

Preferably, the ultrasound may comprise pulsed wave ultrasound. In a highly preferred embodiment, the ultrasound is applied at a power density of 0.7 Wcm-2 or 1.25 Wcm-2 as a continuous wave. Higher power densities may be employed if pulsed wave ultrasound is used.

Use of ultrasound is advantageous as, like light, it may be focused accurately on a target. Moreover, ultrasound is advantageous as it may be focused more deeply into tissues unlike light. It is therefore better suited to whole-tissue penetration (such as but not limited to a lobe of the liver) or whole organ (such as but not limited to the entire liver or an entire muscle, such as the heart) therapy. Another important advantage is that ultrasound is a non-invasive stimulus which is used in a wide variety of diagnostic and therapeutic applications. By way of example, ultrasound is well known in medical imaging techniques and, additionally, in orthopedic therapy. Furthermore, instruments suitable for the application of ultrasound to a subject vertebrate are widely available and their use is well known in the art.

In particular embodiments, the guide molecule is modified by a secondary structure to increase the specificity of the CRISPR-Cas system and the secondary structure can protect against exonuclease activity and allow for 5′ additions to the guide sequence also referred to herein as a protected guide molecule.

In one aspect, the invention provides for hybridizing a “protector RNA” to a sequence of the guide molecule, wherein the “protector RNA” is an RNA strand complementary to the 3′ end of the guide molecule to thereby generate a partially double-stranded guide RNA. In an embodiment of the invention, protecting mismatched bases (i.e. the bases of the guide molecule which do not form part of the guide sequence) with a perfectly complementary protector sequence decreases the likelihood of target RNA binding to the mismatched basepairs at the 3′ end. In particular embodiments of the invention, additional sequences comprising an extented length may also be present within the guide molecule such that the guide comprises a protector sequence within the guide molecule. This “protector sequence” ensures that the guide molecule comprises a “protected sequence” in addition to an “exposed sequence” (comprising the part of the guide sequence hybridizing to the target sequence). In particular embodiments, the guide molecule is modified by the presence of the protector guide to comprise a secondary structure such as a hairpin. Advantageously there are three or four to thirty or more, e.g., about 10 or more, contiguous base pairs having complementarity to the protected sequence, the guide sequence or both. It is advantageous that the protected portion does not impede thermodynamics of the CRISPR-Cas system interacting with its target. By providing such an extension including a partially double stranded guide molecule, the guide molecule is considered protected and results in improved specific binding of the CRISPR-Cas complex, while maintaining specific activity.

In particular embodiments, use is made of a truncated guide (tru-guide), i.e. a guide molecule which comprises a guide sequence which is truncated in length with respect to the canonical guide sequence length. As described by Nowak et al. (Nucleic Acids Res (2016) 44 (20): 9555-9564), such guides may allow catalytically active CRISPR-Cas enzyme to bind its target without cleaving the target RNA. In particular embodiments, a truncated guide is used which allows the binding of the target but retains only nickase activity of the CRISPR-Cas enzyme.

CRISPR RNA-Targeting Effector Proteins

In one example embodiment, the CRISPR system effector protein is an RNA-targeting effector protein. In certain embodiments, the CRISPR system effector protein is a Type VI CRISPR system targeting RNA (e.g., Cas13a, Cas13b, Cas13c or Cas13d). Example RNA-targeting effector proteins include Cas13b and C2c2 (now known as Cas13a). It will be understood that the term “C2c2” herein is used interchangeably with “Cas13a”. “C2c2” is now referred to as “Cas13a”, and the terms are used interchangeably herein unless indicated otherwise. As used herein, the term “Cas13” refers to any Type VI CRISPR system targeting RNA (e.g., Cas13a, Cas13b, Cas13c or Cas13d). When the CRISPR protein is a C2c2 protein, a tracrRNA is not required. C2c2 has been described in Abudayyeh et al. (2016) “C2c2 is a single-component programmable RNA-guided RNA-targeting CRISPR effector”; Science; DOI: 10.1126/science.aaf5573; and Shmakov et al. (2015) “Discovery and Functional Characterization of Diverse Class 2 CRISPR-Cas Systems”, Molecular Cell, DOI: dx.doi.org/10.1016/j.molcel.2015.10.008; which are incorporated herein in their entirety by reference. Cas13b has been described in Smargon et al. (2017) “Cas13b Is a Type VI-B CRISPR-Associated RNA-Guided RNases Differentially Regulated by Accessory Proteins Csx27 and Csx28,” Molecular Cell. 65, 1-13; dx.doi.org/10.1016/j.molcel.2016.12.023., which is incorporated herein in its entirety by reference.

In some embodiments, one or more elements of a nucleic acid-targeting system is derived from a particular organism comprising an endogenous CRISPR RNA-targeting system. In certain example embodiments, the effector protein CRISPR RNA-targeting system comprises at least one HEPN domain, including but not limited to the HEPN domains described herein, HEPN domains known in the art, and domains recognized to be HEPN domains by comparison to consensus sequence motifs. Several such domains are provided herein. In one non-limiting example, a consensus sequence can be derived from the sequences of C2c2 or Cas13b orthologs provided herein. In certain example embodiments, the effector protein comprises a single HEPN domain. In certain other example embodiments, the effector protein comprises two HEPN domains.

In one example embodiment, the effector protein comprise one or more HEPN domains comprising a RxxxxH motif sequence. The RxxxxH motif sequence can be, without limitation, from a HEPN domain described herein or a HEPN domain known in the art. RxxxxH motif sequences further include motif sequences created by combining portions of two or more HEPN domains. As noted, consensus sequences can be derived from the sequences of the orthologs disclosed in U.S. Provisional Patent Application 62/432,240 entitled “Novel CRISPR Enzymes and Systems,” U.S. Provisional Patent Application 62/471,710 entitled “Novel Type VI CRISPR Orthologs and Systems” filed on Mar. 15, 2017, and U.S. Provisional Patent Application entitled “Novel Type VI CRISPR Orthologs and Systems,” labeled as attorney docket number 47627-05-2133 and filed on Apr. 12, 2017.

In certain other example embodiments, the CRISPR system effector protein is a C2c2 nuclease. The activity of C2c2 may depend on the presence of two HEPN domains. These have been shown to be RNase domains, i.e. nuclease (in particular an endonuclease) cutting RNA. C2c2 HEPN may also target DNA, or potentially DNA and/or RNA. On the basis that the HEPN domains of C2c2 are at least capable of binding to and, in their wild-type form, cutting RNA, then it is preferred that the C2c2 effector protein has RNase function. Regarding C2c2 CRISPR systems, reference is made to U.S. Provisional 62/351,662 filed on Jun. 17, 2016 and U.S. Provisional 62/376,377 filed on Aug. 17, 2016. Reference is also made to U.S. Provisional 62/351,803 filed on Jun. 17, 2016. Reference is also made to U.S. Provisional entitled “Novel Crispr Enzymes and Systems” filed Dec. 8, 2016 bearing Broad Institute No. 10035.PA4 and Attorney Docket No. 47627.03.2133. Reference is further made to East-Seletsky et al. “Two distinct RNase activities of CRISPR-C2c2 enable guide-RNA processing and RNA detection” Nature doi:10/1038/nature19802 and Abudayyeh et al. “C2c2 is a single-component programmable RNA-guided RNA targeting CRISPR effector” bioRxiv doi: 10.1101/054742.

In certain embodiments, the C2c2 effector protein is from an organism of a genus selected from the group consisting of: Leptotrichia, Listeria, Corynebacter, Sutterella, Legionella, Treponema, Filifactor, Eubacterium, Streptococcus, Lactobacillus, Mycoplasma, Bacteroides, Flaviivola, Flavobacterium, Sphaerochaeta, Azospirillum, Gluconacetobacter, Neisseria, Roseburia, Parvibaculum, Staphylococcus, Nitratifractor, Mycoplasma, Campylobacter, and Lachnospira, or the C2c2 effector protein is an organism selected from the group consisting of: Leptotrichia shahii, Leptotrichia. wadei, Listeria seeligeri, Clostridium aminophilum, Carnobacterium gallinarum, Paludibacter propionicigenes, Listeria weihenstephanensis, or the C2c2 effector protein is a L. wadei F0279 or L. wadei F0279 (Lw2) C2C2 effector protein. In another embodiment, the one or more guide RNAs are designed to detect a single nucleotide polymorphism, splice variant of a transcript, or a frameshift mutation in a target RNA or DNA.

In certain example embodiments, the RNA-targeting effector protein is a Type VI-B effector protein, such as Cas13b and Group 29 or Group 30 proteins. In certain example embodiments, the RNA-targeting effector protein comprises one or more HEPN domains. In certain example embodiments, the RNA-targeting effector protein comprises a C-terminal HEPN domain, a N-terminal HEPN domain, or both. Regarding example Type VI-B effector proteins that may be used in the context of this invention, reference is made to U.S. application Ser. No. 15/331,792 entitled “Novel CRISPR Enzymes and Systems” and filed Oct. 21, 2016, International Patent Application No. PCT/US2016/058302 entitled “Novel CRISPR Enzymes and Systems”, and filed Oct. 21, 2016, and Smargon et al. “Cas13b is a Type VI-B CRISPR-associated RNA-Guided RNase differentially regulated by accessory proteins Csx27 and Csx28” Molecular Cell, 65, 1-13 (2017); dx.doi.org/10.1016/j.molcel.2016.12.023, and U.S. Provisional Application No. to be assigned, entitled “Novel Cas13b Orthologues CRISPR Enzymes and System” filed Mar. 15, 2017. In particular embodiments, the Cas13b enzyme is derived from Bergeyella zoohelcum.

In certain example embodiments, the RNA-targeting effector protein is a Cas13c effector protein as disclosed in U.S. Provisional Patent Application No. 62/525,165 filed Jun. 26, 2017, and PCT Application No. US 2017/047193 filed Aug. 16, 2017.

In some embodiments, one or more elements of a nucleic acid-targeting system is derived from a particular organism comprising an endogenous CRISPR RNA-targeting system. In certain embodiments, the CRISPR RNA-targeting system is found in Eubacterium and Ruminococcus. In certain embodiments, the effector protein comprises targeted and collateral ssRNA cleavage activity. In certain embodiments, the effector protein comprises dual HEPN domains. In certain embodiments, the effector protein lacks a counterpart to the Helical-1 domain of Cas13a. In certain embodiments, the effector protein is smaller than previously characterized class 2 CRISPR effectors, with a median size of 928 aa. This median size is 190 aa (17%) less than that of Cas13c, more than 200 aa (18%) less than that of Cas13b, and more than 300 aa (26%) less than that of Cas13a. In certain embodiments, the effector protein has no requirement for a flanking sequence (e.g., PFS, PAM).

In certain embodiments, the effector protein locus structures include a WYL domain containing accessory protein (so denoted after three amino acids that were conserved in the originally identified group of these domains; see, e.g., WYL domain IPR026881). In certain embodiments, the WYL domain accessory protein comprises at least one helix-turn-helix (HTH) or ribbon-helix-helix (RHH) DNA-binding domain. In certain embodiments, the WYL domain containing accessory protein increases both the targeted and the collateral ssRNA cleavage activity of the RNA-targeting effector protein. In certain embodiments, the WYL domain containing accessory protein comprises an N-terminal RHH domain, as well as a pattern of primarily hydrophobic conserved residues, including an invariant tyrosine-leucine doublet corresponding to the original WYL motif. In certain embodiments, the WYL domain containing accessory protein is WYL1. WYL1 is a single WYL-domain protein associated primarily with Ruminococcus.

In other example embodiments, the Type VI RNA-targeting Cas enzyme is Cas13d. In certain embodiments, Cas13d is Eubacterium siraeum DSM 15702 (EsCas13d) or Ruminococcus sp. N15.MGS-57 (RspCas13d) (see, e.g., Yan et al., Cas13d Is a Compact RNA-Targeting Type VI CRISPR Effector Positively Modulated by a WYL-Domain-Containing Accessory Protein, Molecular Cell (2018), doi.org/10.1016/j.molcel.2018.02.028). RspCas13d and EsCas13d have no flanking sequence requirements (e.g., PFS, PAM).

Cas13 RNA Editing

In one aspect, the invention provides a method of modifying or editing a target transcript in a eukaryotic cell. In some embodiments, the method comprises allowing a CRISPR-Cas effector module complex to bind to the target polynucleotide to effect RNA base editing, wherein the CRISPR-Cas effector module complex comprises a Cas effector module complexed with a guide sequence hybridized to a target sequence within said target polynucleotide, wherein said guide sequence is linked to a direct repeat sequence. In some embodiments, the Cas effector module comprises a catalytically inactive CRISPR-Cas protein. In some embodiments, the guide sequence is designed to introduce one or more mismatches to the RNA/RNA duplex formed between the target sequence and the guide sequence. In particular embodiments, the mismatch is an A-C mismatch. In some embodiments, the Cas effector may associate with one or more functional domains (e.g. via fusion protein or suitable linkers). In some embodiments, the effector domain comprises one or more cytindine or adenosine deaminases that mediate endogenous editing of via hydrolytic deamination. In particular embodiments, the effector domain comprises the adenosine deaminase acting on RNA (ADAR) family of enzymes. In particular embodiments, the adenosine deaminase protein or catalytic domain thereof capable of deaminating adenosine or cytidine in RNA or is an RNA specific adenosine deaminase and/or is a bacterial, human, cephalopod, or Drosophila adenosine deaminase protein or catalytic domain thereof, preferably TadA, more preferably ADAR, optionally huADAR, optionally (hu)ADAR1 or (hu)ADAR2, preferably huADAR2 or catalytic domain thereof.

The present application relates to modifying a target RNA sequence of interest (see, e.g, Cox et al., Science. 2017 Nov. 24; 358(6366):1019-1027). Using RNA-targeting rather than DNA targeting offers several advantages relevant for therapeutic development. First, there are substantial safety benefits to targeting RNA: there will be fewer off-target events because the available sequence space in the transcriptome is significantly smaller than the genome, and if an off-target event does occur, it will be transient and less likely to induce negative side effects. Second, RNA-targeting therapeutics will be more efficient because they are cell-type independent and not have to enter the nucleus, making them easier to deliver.

A further aspect of the invention relates to the method and composition as envisaged herein for use in prophylactic or therapeutic treatment, preferably wherein said target locus of interest is within a human or animal and to methods of modifying an Adenine or Cytidine in a target RNA sequence of interest, comprising delivering to said target RNA, the composition as described herein. In particular embodiments, the CRISPR system and the adenonsine deaminase, or catalytic domain thereof, are delivered as one or more polynucleotide molecules, as a ribonucleoprotein complex, optionally via particles, vesicles, or one or more viral vectors. In particular embodiments, the invention thus comprises compositions for use in therapy. This implies that the methods can be performed in vivo, ex vivo or in vitro. In particular embodiments, when the target is a human or animal target, the method is carried out ex vivo or in vitro.

A further aspect of the invention relates to the method as envisaged herein for use in prophylactic or therapeutic treatment, preferably wherein said target of interest is within a human or animal and to methods of modifying an Adenine or Cytidine in a target RNA sequence of interest, comprising delivering to said target RNA, the composition as described herein. In particular embodiments, the CRISPR system and the adenonsine deaminase, or catalytic domain thereof, are delivered as one or more polynucleotide molecules, as a ribonucleoprotein complex, optionally via particles, vesicles, or one or more viral vectors.

In one aspect, the invention provides a method of generating a eukaryotic cell comprising a modified or edited gene. In some embodiments, the method comprises (a) introducing one or more vectors into a eukaryotic cell, wherein the one or more vectors drive expression of one or more of: Cas effector module, and a guide sequence linked to a direct repeat sequence, wherein the Cas effector module associate one or more effector domains that mediate base editing, and (b) allowing a CRISPR-Cas effector module complex to bind to a target polynucleotide to effect base editing of the target polynucleotide within said disease gene, wherein the CRISPR-Cas effector module complex comprises a Cas effector module complexed with the guide sequence that is hybridized to the target sequence within the target polynucleotide, wherein the guide sequence may be designed to introduce one or more mismatches between the RNA/RNA duplex formed between the guide sequence and the target sequence. In particular embodiments, the mismatch is an A-C mismatch. In some embodiments, the Cas effector may associate with one or more functional domains (e.g. via fusion protein or suitable linkers). In some embodiments, the effector domain comprises one or more cytidine or adenosine deaminases that mediate endogenous editing of via hydrolytic deamination. In particular embodiments, the effector domain comprises the adenosine deaminase acting on RNA (ADAR) family of enzymes. In particular embodiments, the adenosine deaminase protein or catalytic domain thereof capable of deaminating adenosine or cytidine in RNA or is an RNA specific adenosine deaminase and/or is a bacterial, human, cephalopod, or Drosophila adenosine deaminase protein or catalytic domain thereof, preferably TadA, more preferably ADAR, optionally huADAR, optionally (hu)ADAR1 or (hu)ADAR2, preferably huADAR2 or catalytic domain thereof.

A further aspect relates to an isolated cell obtained or obtainable from the methods described herein comprising the composition described herein or progeny of said modified cell, preferably wherein said cell comprises a hypoxanthine or a guanine in replace of said Adenine in said target RNA of interest compared to a corresponding cell not subjected to the method. In particular embodiments, the cell is a eukaryotic cell, preferably a human or non-human animal cell, optionally a therapeutic T cell or an antibody-producing B-cell.

In some embodiments, the modified cell is a therapeutic T cell, such as a T cell suitable for adoptive cell transfer therapies (e.g., CAR-T therapies). The modification may result in one or more desirable traits in the therapeutic T cell, as described further herein.

The invention further relates to a method for cell therapy, comprising administering to a patient in need thereof the modified cell described herein, wherein the presence of the modified cell remedies a disease in the patient. In one embodiment, the modified cell for cell therapy is a epithelial cell (e.g., tuft cell).

The present invention may be further illustrated and extended based on aspects of CRISPR-Cas development and use as set forth in the following articles and particularly as relates to delivery of a CRISPR protein complex and uses of an RNA guided endonuclease in cells and organisms:

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each of which is incorporated herein by reference, may be considered in the practice of the instant invention, and discussed briefly below:

-   -   Cong et al. engineered type II CRISPR-Cas systems for use in         eukaryotic cells based on both Streptococcus thermophilus Cas9         and also Streptococcus pyogenes Cas9 and demonstrated that Cas9         nucleases can be directed by short RNAs to induce precise         cleavage of DNA in human and mouse cells. Their study further         showed that Cas9 as converted into a nicking enzyme can be used         to facilitate homology-directed repair in eukaryotic cells with         minimal mutagenic activity. Additionally, their study         demonstrated that multiple guide sequences can be encoded into a         single CRISPR array to enable simultaneous editing of several at         endogenous genomic loci sites within the mammalian genome,         demonstrating easy programmability and wide applicability of the         RNA-guided nuclease technology. This ability to use RNA to         program sequence specific DNA cleavage in cells defined a new         class of genome engineering tools. These studies further showed         that other CRISPR loci are likely to be transplantable into         mammalian cells and can also mediate mammalian genome cleavage.         Importantly, it can be envisaged that several aspects of the         CRISPR-Cas system can be further improved to increase its         efficiency and versatility.     -   Jiang et al. used the clustered, regularly interspaced, short         palindromic repeats (CRISPR)-associated Cas9 endonuclease         complexed with dual-RNAs to introduce precise mutations in the         genomes of Streptococcus pneumoniae and Escherichia coli. The         approach relied on dual-RNA:Cas9-directed cleavage at the         targeted genomic site to kill unmutated cells and circumvents         the need for selectable markers or counter-selection systems.         The study reported reprogramming dual-RNA:Cas9 specificity by         changing the sequence of short CRISPR RNA (crRNA) to make         single- and multinucleotide changes carried on editing         templates. The study showed that simultaneous use of two crRNAs         enabled multiplex mutagenesis. Furthermore, when the approach         was used in combination with recombineering, in S. pneumoniae,         nearly 100% of cells that were recovered using the described         approach contained the desired mutation, and in E. coli, 65%         that were recovered contained the mutation.     -   Wang et al. (2013) used the CRISPR-Cas system for the one-step         generation of mice carrying mutations in multiple genes which         were traditionally generated in multiple steps by sequential         recombination in embryonic stem cells and/or time-consuming         intercrossing of mice with a single mutation. The CRISPR-Cas         system will greatly accelerate the in vivo study of functionally         redundant genes and of epistatic gene interactions.     -   Konermann et al. (2013) addressed the need in the art for         versatile and robust technologies that enable optical and         chemical modulation of DNA-binding domains based CRISPR Cas9         enzyme and also Transcriptional Activator Like Effectors     -   Ran et al. (2013-A) described an approach that combined a Cas9         nickase mutant with paired guide RNAs to introduce targeted         double-strand breaks. This addresses the issue of the Cas9         nuclease from the microbial CRISPR-Cas system being targeted to         specific genomic loci by a guide sequence, which can tolerate         certain mismatches to the DNA target and thereby promote         undesired off-target mutagenesis. Because individual nicks in         the genome are repaired with high fidelity, simultaneous nicking         via appropriately offset guide RNAs is required for         double-stranded breaks and extends the number of specifically         recognized bases for target cleavage. The authors demonstrated         that using paired nicking can reduce off-target activity by 50-         to 1,500-fold in cell lines and to facilitate gene knockout in         mouse zygotes without sacrificing on-target cleavage efficiency.         This versatile strategy enables a wide variety of genome editing         applications that require high specificity.     -   Hsu et al. (2013) characterized SpCas9 targeting specificity in         human cells to inform the selection of target sites and avoid         off-target effects. The study evaluated >700 guide RNA variants         and SpCas9-induced indel mutation levels at >100 predicted         genomic off-target loci in 293T and 293FT cells. The authors         that SpCas9 tolerates mismatches between guide RNA and target         DNA at different positions in a sequence-dependent manner,         sensitive to the number, position and distribution of         mismatches. The authors further showed that SpCas9-mediated         cleavage is unaffected by DNA methylation and that the dosage of         SpCas9 and guide RNA can be titrated to minimize off-target         modification. Additionally, to facilitate mammalian genome         engineering applications, the authors reported providing a         web-based software tool to guide the selection and validation of         target sequences as well as off-target analyses.     -   Ran et al. (2013-B) described a set of tools for Cas9-mediated         genome editing via non-homologous end joining (NHEJ) or         homology-directed repair (HDR) in mammalian cells, as well as         generation of modified cell lines for downstream functional         studies. To minimize off-target cleavage, the authors further         described a double-nicking strategy using the Cas9 nickase         mutant with paired guide RNAs. The protocol provided by the         authors experimentally derived guidelines for the selection of         target sites, evaluation of cleavage efficiency and analysis of         off-target activity. The studies showed that beginning with         target design, gene modifications can be achieved within as         little as 1-2 weeks, and modified clonal cell lines can be         derived within 2-3 weeks.     -   Shalem et al. described a new way to interrogate gene function         on a genome-wide scale. Their studies showed that delivery of a         genome-scale CRISPR-Cas9 knockout (GeCKO) library targeted         18,080 genes with 64,751 unique guide sequences enabled both         negative and positive selection screening in human cells. First,         the authors showed use of the GeCKO library to identify genes         essential for cell viability in cancer and pluripotent stem         cells. Next, in a melanoma model, the authors screened for genes         whose loss is involved in resistance to vemurafenib, a         therapeutic that inhibits mutant protein kinase BRAF. Their         studies showed that the highest-ranking candidates included         previously validated genes NF1 and MED12 as well as novel hits         NF2, CUL3, TADA2B, and TADA1. The authors observed a high level         of consistency between independent guide RNAs targeting the same         gene and a high rate of hit confirmation, and thus demonstrated         the promise of genome-scale screening with Cas9.

-   Nishimasu et al. reported the crystal structure of     Streptococcuspyogenes Cas9 in complex with sgRNA and its target DNA     at 2.5 A° resolution. The structure revealed a bilobed architecture     composed of target recognition and nuclease lobes, accommodating the     sgRNA:DNA heteroduplex in a positively charged groove at their     interface. Whereas the recognition lobe is essential for binding     sgRNA and DNA, the nuclease lobe contains the HNH and RuvC nuclease     domains, which are properly positioned for cleavage of the     complementary and non-complementary strands of the target DNA,     respectively. The nuclease lobe also contains a carboxyl-terminal     domain responsible for the interaction with the protospacer adjacent     motif (PAM). This high-resolution structure and accompanying     functional analyses have revealed the molecular mechanism of     RNA-guided DNA targeting by Cas9, thus paving the way for the     rational design of new, versatile genome-editing technologies.     -   Wu et al. mapped genome-wide binding sites of a catalytically         inactive Cas9 (dCas9) from Streptococcus pyogenes loaded with         single guide RNAs (sgRNAs) in mouse embryonic stem cells         (mESCs). The authors showed that each of the four sgRNAs tested         targets dCas9 to between tens and thousands of genomic sites,         frequently characterized by a 5-nucleotide seed region in the         sgRNA and an NGG protospacer adjacent motif (PAM). Chromatin         inaccessibility decreases dCas9 binding to other sites with         matching seed sequences; thus 70% of off-target sites are         associated with genes. The authors showed that targeted         sequencing of 295 dCas9 binding sites in mESCs transfected with         catalytically active Cas9 identified only one site mutated above         background levels. The authors proposed a two-state model for         Cas9 binding and cleavage, in which a seed match triggers         binding but extensive pairing with target DNA is required for         cleavage.     -   Platt et al. established a Cre-dependent Cas9 knockin mouse. The         authors demonstrated in vivo as well as ex vivo genome editing         using adeno-associated virus (AAV)-, lentivirus-, or         particle-mediated delivery of guide RNA in neurons, immune         cells, and endothelial cells.     -   Hsu et al. (2014) is a review article that discusses generally         CRISPR-Cas9 history from yogurt to genome editing, including         genetic screening of cells.     -   Wang et al. (2014) relates to a pooled, loss-of-function genetic         screening approach suitable for both positive and negative         selection that uses a genome-scale lentiviral single guide RNA         (sgRNA) library.     -   Doench et al. created a pool of sgRNAs, tiling across all         possible target sites of a panel of six endogenous mouse and         three endogenous human genes and quantitatively assessed their         ability to produce null alleles of their target gene by antibody         staining and flow cytometry. The authors showed that         optimization of the PAM improved activity and also provided an         on-line tool for designing sgRNAs.     -   Swiech et al. demonstrate that AAV-mediated SpCas9 genome         editing can enable reverse genetic studies of gene function in         the brain.     -   Konermann et al. (2015) discusses the ability to attach multiple         effector domains, e.g., transcriptional activator, functional         and epigenomic regulators at appropriate positions on the guide         such as stem or tetraloop with and without linkers.     -   Zetsche et al. demonstrates that the Cas9 enzyme can be split         into two and hence the assembly of Cas9 for activation can be         controlled.     -   Chen et al. relates to multiplex screening by demonstrating that         a genome-wide in vivo CRISPR-Cas9 screen in mice reveals genes         regulating lung metastasis.     -   Ran et al. (2015) relates to SaCas9 and its ability to edit         genomes and demonstrates that one cannot extrapolate from         biochemical assays.     -   Shalem et al. (2015) described ways in which catalytically         inactive Cas9 (dCas9) fusions are used to synthetically repress         (CRISPRi) or activate (CRISPRa) expression, showing. advances         using Cas9 for genome-scale screens, including arrayed and         pooled screens, knockout approaches that inactivate genomic loci         and strategies that modulate transcriptional activity.     -   Xu et al. (2015) assessed the DNA sequence features that         contribute to single guide RNA (sgRNA) efficiency in         CRISPR-based screens. The authors explored efficiency of         CRISPR-Cas9 knockout and nucleotide preference at the cleavage         site. The authors also found that the sequence preference for         CRISPRi/a is substantially different from that for CRISPR-Cas9         knockout.     -   Parnas et al. (2015) introduced genome-wide pooled CRISPR-Cas9         libraries into dendritic cells (DCs) to identify genes that         control the induction of tumor necrosis factor (Tnf) by         bacterial lipopolysaccharide (LPS). Known regulators of Tlr4         signaling and previously unknown candidates were identified and         classified into three functional modules with distinct effects         on the canonical responses to LPS.     -   Ramanan et al (2015) demonstrated cleavage of viral episomal DNA         (cccDNA) in infected cells. The HBV genome exists in the nuclei         of infected hepatocytes as a 3.2 kb double-stranded episomal DNA         species called covalently closed circular DNA (cccDNA), which is         a key component in the HBV life cycle whose replication is not         inhibited by current therapies. The authors showed that sgRNAs         specifically targeting highly conserved regions of HBV robustly         suppresses viral replication and depleted cccDNA.     -   Nishimasu et al. (2015) reported the crystal structures of         SaCas9 in complex with a single guide RNA (sgRNA) and its         double-stranded DNA targets, containing the 5′-TTGAAT-3′ PAM and         the 5′-TTGGGT-3′ PAM. A structural comparison of SaCas9 with         SpCas9 highlighted both structural conservation and divergence,         explaining their distinct PAM specificities and orthologous         sgRNA recognition.     -   Canver et al. (2015) demonstrated a CRISPR-Cas9-based functional         investigation of non-coding genomic elements. The authors         developed pooled CRISPR-Cas9 guide RNA libraries to perform in         situ saturating mutagenesis of the human and mouse BCL11A         enhancers which revealed critical features of the enhancers.     -   Zetsche et al. (2015) reported characterization of Cpf1, a class         2 CRISPR nuclease from Francisella novicida U112 having features         distinct from Cas9. Cpf1 is a single RNA-guided endonuclease         lacking tracrRNA, utilizes a T-rich protospacer-adjacent motif,         and cleaves DNA via a staggered DNA double-stranded break.     -   Shmakov et al. (2015) reported three distinct Class 2 CRISPR-Cas         systems. Two system CRISPR enzymes (C2cl and C2c3) contain         RuvC-like endonuclease domains distantly related to Cpf1. Unlike         Cpf1, C2cl depends on both crRNA and tracrRNA for DNA cleavage.         The third enzyme (C2c2) contains two predicted HEPN RNase         domains and is tracrRNA independent.     -   Slaymaker et al (2016) reported the use of structure-guided         protein engineering to improve the specificity of Streptococcus         pyogenes Cas9 (SpCas9). The authors developed “enhanced         specificity” SpCas9 (eSpCas9) variants which maintained robust         on-target cleavage with reduced off-target effects.     -   Cox et al., (2017) reported the use of catalytically inactive         Cas13 (dCas13) to direct adenosine-to-inosine deaminase activity         by ADAR2 (adenosine deaminase acting on RNA type 2) to         transcripts in mammalian cells. The system, referred to as RNA         Editing for Programmable A to I Replacement (REPAIR), has no         strict sequence constraints and can be used to edit full-length         transcripts. The authors further engineered the system to create         a high-specificity variant and minimized the system to         facilitate viral delivery.

The methods and tools provided herein are may be designed for use with or Cas13, a type II nuclease that does not make use of tracrRNA. Orthologs of Cas13 have been identified in different bacterial species as described herein. Further type II nucleases with similar properties can be identified using methods described in the art (Shmakov et al. 2015, 60:385-397; Abudayeh et al. 2016, Science, 5; 353(6299)). In particular embodiments, such methods for identifying novel CRISPR effector proteins may comprise the steps of selecting sequences from the database encoding a seed which identifies the presence of a CRISPR Cas locus, identifying loci located within 10 kb of the seed comprising Open Reading Frames (ORFs) in the selected sequences, selecting therefrom loci comprising ORFs of which only a single ORF encodes a novel CRISPR effector having greater than 700 amino acids and no more than 90% homology to a known CRISPR effector. In particular embodiments, the seed is a protein that is common to the CRISPR-Cas system, such as Cas1. In further embodiments, the CRISPR array is used as a seed to identify new effector proteins.

Also, “Dimeric CRISPR RNA-guided FokI nucleases for highly specific genome editing”, Shengdar Q. Tsai, Nicolas Wyvekens, Cyd Khayter, Jennifer A. Foden, Vishal Thapar, Deepak Reyon, Mathew J. Goodwin, Martin J. Aryee, J. Keith Joung Nature Biotechnology 32(6): 569-77 (2014), relates to dimeric RNA-guided FokI Nucleases that recognize extended sequences and can edit endogenous genes with high efficiencies in human cells.

With respect to general information on CRISPR/Cas Systems, components thereof, and delivery of such components, including methods, materials, delivery vehicles, vectors, particles, and making and using thereof, including as to amounts and formulations, as well as CRISPR-Cas-expressing eukaryotic cells, CRISPR-Cas expressing eukaryotes, such as a mouse, reference is made to: U.S. Pat. Nos. 8,999,641, 8,993,233, 8,697,359, 8,771,945, 8,795,965, 8,865,406, 8,871,445, 8,889,356, 8,889,418, 8,895,308, 8,906,616, 8,932,814, and 8,945,839; US Patent Publications US 2014-0310830 (U.S. application Ser. No. 14/105,031), US 2014-0287938 A1 (U.S. application Ser. No. 14/213,991), US 2014-0273234 A1 (U.S. application Ser. No. 14/293,674), US2014-0273232 A1 (U.S. application Ser. No. 14/290,575), US 2014-0273231 (U.S. application Ser. No. 14/259,420), US 2014-0256046 A1 (U.S. application Ser. No. 14/226,274), US 2014-0248702 A1 (U.S. application Ser. No. 14/258,458), US 2014-0242700 A1 (U.S. application Ser. No. 14/222,930), US 2014-0242699 A1 (U.S. application Ser. No. 14/183,512), US 2014-0242664 A1 (U.S. application Ser. No. 14/104,990), US 2014-0234972 A1 (U.S. application Ser. No. 14/183,471), US 2014-0227787 A1 (U.S. application Ser. No. 14/256,912), US 2014-0189896 A1 (U.S. application Ser. No. 14/105,035), US 2014-0186958 (U.S. application Ser. No. 14/105,017), US 2014-0186919 A1 (U.S. application Ser. No. 14/104,977), US 2014-0186843 A1 (U.S. application Ser. No. 14/104,900), US 2014-0179770 A1 (U.S. application Ser. No. 14/104,837) and US 2014-0179006 A1 (U.S. application Ser. No. 14/183,486), US 2014-0170753 (U.S. application Ser. No. 14/183,429); US 2015-0184139 (U.S. application Ser. No. 14/324,960); Ser. No. 14/054,414 European Patent Applications EP 2 771 468 (EP13818570.7), EP 2 764 103 (EP13824232.6), and EP 2 784 162 (EP14170383.5); and PCT Patent Publications WO2014/093661 (PCT/US2013/074743), WO2014/093694 (PCT/US2013/074790), WO2014/093595 (PCT/US2013/074611), WO2014/093718 (PCT/US2013/074825), WO2014/093709 (PCT/US2013/074812), WO2014/093622 (PCT/US2013/074667), WO2014/093635 (PCT/US2013/074691), WO2014/093655 (PCT/US2013/074736), WO2014/093712 (PCT/US2013/074819), WO2014/093701 (PCT/US2013/074800), WO2014/018423 (PCT/US2013/051418), WO2014/204723 (PCT/US2014/041790), WO2014/204724 (PCT/US2014/041800), WO2014/204725 (PCT/US2014/041803), WO2014/204726 (PCT/US2014/041804), WO2014/204727 (PCT/US2014/041806), WO2014/204728 (PCT/US2014/041808), WO2014/204729 (PCT/US2014/041809), WO2015/089351 (PCT/US2014/069897), WO2015/089354 (PCT/US2014/069902), WO2015/089364 (PCT/US2014/069925), WO2015/089427 (PCT/US2014/070068), WO2015/089462 (PCT/US2014/070127), WO2015/089419 (PCT/US2014/070057), WO2015/089465 (PCT/US2014/070135), WO2015/089486 (PCT/US2014/070175), WO2015/058052 (PCT/US2014/061077), WO2015/070083 (PCT/US2014/064663), WO2015/089354 (PCT/US2014/069902), WO2015/089351 (PCT/US2014/069897), WO2015/089364 (PCT/US2014/069925), WO2015/089427 (PCT/US2014/070068), WO2015/089473 (PCT/US2014/070152), WO2015/089486 (PCT/US2014/070175), WO2016/049258 (PCT/US2015/051830), WO2016/094867 (PCT/US2015/065385), WO2016/094872 (PCT/US2015/065393), WO2016/094874 (PCT/US2015/065396), WO2016/106244 (PCT/US2015/067177).

Mention is also made of U.S. application 62/180,709, 17-Jun.-15, PROTECTED GUIDE RNAS (PGRNAS); U.S. application 62/091,455, filed, 12-Dec.-14, PROTECTED GUIDE RNAS (PGRNAS); U.S. application 62/096,708, 24-Dec.-14, PROTECTED GUIDE RNAS (PGRNAS); U.S. applications 62/091,462, 12-Dec.-14, 62/096,324, 23-Dec.-14, 62/180,681, 17 Jun. 2015, and 62/237,496, 5 Oct. 2015, DEAD GUIDES FOR CRISPR TRANSCRIPTION FACTORS; U.S. application 62/091,456, 12-Dec.-14 and 62/180,692, 17 Jun. 2015, ESCORTED AND FUNCTIONALIZED GUIDES FOR CRISPR-CAS SYSTEMS; U.S. application 62/091,461, 12-Dec.-14, DELIVERY, USE AND THERAPEUTIC APPLICATIONS OF THE CRISPR-CAS SYSTEMS AND COMPOSITIONS FOR GENOME EDITING AS TO HEMATOPOETIC STEM CELLS (HSCs); U.S. application 62/094,903, 19-Dec.-14, UNBIASED IDENTIFICATION OF DOUBLE-STRAND BREAKS AND GENOMIC REARRANGEMENT BY GENOME-WISE INSERT CAPTURE SEQUENCING; U.S. application 62/096,761, 24-Dec.-14, ENGINEERING OF SYSTEMS, METHODS AND OPTIMIZED ENZYME AND GUIDE SCAFFOLDS FOR SEQUENCE MANIPULATION; U.S. application 62/098,059, 30-Dec.-14, 62/181,641, 18 Jun. 2015, and 62/181,667, 18 Jun. 2015, RNA-TARGETING SYSTEM; U.S. application 62/096,656, 24-Dec.-14 and 62/181,151, 17 Jun. 2015, CRISPR HAVING OR ASSOCIATED WITH DESTABILIZATION DOMAINS; U.S. application 62/096,697, 24-Dec.-14, CRISPR HAVING OR ASSOCIATED WITH AAV; U.S. application 62/098,158, 30-Dec.-14, ENGINEERED CRISPR COMPLEX INSERTIONAL TARGETING SYSTEMS; U.S. application 62/151,052, 22-Apr.-15, CELLULAR TARGETING FOR EXTRACELLULAR EXOSOMAL REPORTING; U.S. application 62/054,490, 24-Sep.-14, DELIVERY, USE AND THERAPEUTIC APPLICATIONS OF THE CRISPR-CAS SYSTEMS AND COMPOSITIONS FOR TARGETING DISORDERS AND DISEASES USING PARTICLE DELIVERY COMPONENTS; U.S. application 61/939,154, 12-F EB-14, SYSTEMS, METHODS AND COMPOSITIONS FOR SEQUENCE MANIPULATION WITH OPTIMIZED FUNCTIONAL CRISPR-CAS SYSTEMS; U.S. application 62/055,484, 25-Sep.-14, SYSTEMS, METHODS AND COMPOSITIONS FOR SEQUENCE MANIPULATION WITH OPTIMIZED FUNCTIONAL CRISPR-CAS SYSTEMS; U.S. application 62/087,537, 4-Dec.-14, SYSTEMS, METHODS AND COMPOSITIONS FOR SEQUENCE MANIPULATION WITH OPTIMIZED FUNCTIONAL CRISPR-CAS SYSTEMS; U.S. application 62/054,651, 24-Sep.-14, DELIVERY, USE AND THERAPEUTIC APPLICATIONS OF THE CRISPR-CAS SYSTEMS AND COMPOSITIONS FOR MODELING COMPETITION OF MULTIPLE CANCER MUTATIONS IN VIVO; U.S. application 62/067,886, 23-Oct.-14, DELIVERY, USE AND THERAPEUTIC APPLICATIONS OF THE CRISPR-CAS SYSTEMS AND COMPOSITIONS FOR MODELING COMPETITION OF MULTIPLE CANCER MUTATIONS IN VIVO; U.S. applications 62/054,675, 24-Sep.-14 and 62/181,002, 17 Jun. 2015, DELIVERY, USE AND THERAPEUTIC APPLICATIONS OF THE CRISPR-CAS SYSTEMS AND COMPOSITIONS IN NEURONAL CELLS/TISSUES; U.S. application 62/054,528, 24-Sep.-14, DELIVERY, USE AND THERAPEUTIC APPLICATIONS OF THE CRISPR-CAS SYSTEMS AND COMPOSITIONS IN IMMUNE DISEASES OR DISORDERS; U.S. application 62/055,454, 25-Sep.-14, DELIVERY, USE AND THERAPEUTIC APPLICATIONS OF THE CRISPR-CAS SYSTEMS AND COMPOSITIONS FOR TARGETING DISORDERS AND DISEASES USING CELL PENETRATION PEPTIDES (CPP); U.S. application 62/055,460, 25-Sep.-14, MULTIFUNCTIONAL-CRISPR COMPLEXES AND/OR OPTIMIZED ENZYME LINKED FUNCTIONAL-CRISPR COMPLEXES; U.S. application 62/087,475, 4-Dec.-14 and 62/181,690, 18 Jun. 2015, FUNCTIONAL SCREENING WITH OPTIMIZED FUNCTIONAL CRISPR-CAS SYSTEMS; U.S. application 62/055,487, 25-Sep.-14, FUNCTIONAL SCREENING WITH OPTIMIZED FUNCTIONAL CRISPR-CAS SYSTEMS; U.S. application 62/087,546, 4-Dec.-14 and 62/181,687, 18 Jun. 2015, MULTIFUNCTIONAL CRISPR COMPLEXES AND/OR OPTIMIZED ENZYME LINKED FUNCTIONAL-CRISPR COMPLEXES; and U.S. application 62/098,285, 30-Dec.-14, CRISPR MEDIATED IN VIVO MODELING AND GENETIC SCREENING OF TUMOR GROWTH AND METASTASIS.

Mention is made of U.S. applications 62/181,659, 18 Jun. 2015 and 62/207,318, 19 Aug. 2015, ENGINEERING AND OPTIMIZATION OF SYSTEMS, METHODS, ENZYME AND GUIDE SCAFFOLDS OF CAS9 ORTHOLOGS AND VARIANTS FOR SEQUENCE MANIPULATION. Mention is made of U.S. applications 62/181,663, 18 Jun. 2015 and 62/245,264, 22 Oct. 2015, NOVEL CRISPR ENZYMES AND SYSTEMS, U.S. applications 62/181,675, 18 Jun. 2015, 62/285,349, 22 Oct. 2015, 62/296,522, 17 Feb. 2016, and 62/320,231, 8 Apr. 2016, NOVEL CRISPR ENZYMES AND SYSTEMS, U.S. application 62/232,067, 24 Sep. 2015, U.S. application Ser. No. 14/975,085, 18 Dec. 2015, European application No. 16150428.7, U.S. application 62/205,733, 16 Aug. 2015, U.S. application 62/201,542, 5 Aug. 2015, U.S. application 62/193,507, 16 Jul. 2015, and U.S. application 62/181,739, 18 Jun. 2015, each entitled NOVEL CRISPR ENZYMES AND SYSTEMS and of U.S. application 62/245,270, 22 Oct. 2015, NOVEL CRISPR ENZYMES AND SYSTEMS. Mention is also made of U.S. application 61/939,256, 12 Feb. 2014, and WO 2015/089473 (PCT/US2014/070152), 12 Dec. 2014, each entitled ENGINEERING OF SYSTEMS, METHODS AND OPTIMIZED GUIDE COMPOSITIONS WITH NEW ARCHITECTURES FOR SEQUENCE MANIPULATION. Mention is also made of PCT/US2015/045504, 15 Aug. 2015, U.S. application 62/180,699, 17 Jun. 2015, and U.S. application 62/038,358, 17 Aug. 2014, each entitled GENOME EDITING USING CAS9 NICKASES.

Each of these patents, patent publications, and applications, and all documents cited therein or during their prosecution (“appln cited documents”) and all documents cited or referenced in the appln cited documents, together with any instructions, descriptions, product specifications, and product sheets for any products mentioned therein or in any document therein and incorporated by reference herein, are hereby incorporated herein by reference, and may be employed in the practice of the invention. All documents (e.g., these patents, patent publications and applications and the appln cited documents) are incorporated herein by reference to the same extent as if each individual document was specifically and individually indicated to be incorporated by reference.

In particular embodiments, pre-complexed guide RNA and CRISPR effector protein, (optionally, adenosine deaminase fused to a CRISPR protein or an adaptor) are delivered as a ribonucleoprotein (RNP). RNPs have the advantage that they lead to rapid editing effects even more so than the RNA method because this process avoids the need for transcription. An important advantage is that both RNP delivery is transient, reducing off-target effects and toxicity issues. Efficient genome editing in different cell types has been observed by Kim et al. (2014, Genome Res. 24(6):1012-9), Paix et al. (2015, Genetics 204(1):47-54), Chu et al. (2016, BMC Biotechnol. 16:4), and Wang et al. (2013, Cell. 9; 153(4):910-8).

In particular embodiments, the ribonucleoprotein is delivered byway of a polypeptide-based shuttle agent as described in WO2016161516. WO2016161516 describes efficient transduction of polypeptide cargos using synthetic peptides comprising an endosome leakage domain (ELD) operably linked to a cell penetrating domain (CPD), to a histidine-rich domain and a CPD. Similarly these polypeptides can be used for the delivery of CRISPR-effector based RNPs in eukaryotic cells.

Tale Systems

As disclosed herein editing can be made by way of the transcription activator-like effector nucleases (TALENs) system. Transcription activator-like effectors (TALEs) can be engineered to bind practically any desired DNA sequence. Exemplary methods of genome editing using the TALEN system can be found for example in Cermak T. Doyle E L. Christian M. Wang L. Zhang Y. Schmidt C, et al. Efficient design and assembly of custom TALEN and other TAL effector-based constructs for DNA targeting. Nucleic Acids Res. 2011; 39:e82; Zhang F. Cong L. Lodato S. Kosuri S. Church G M. Arlotta P Efficient construction of sequence-specific TAL effectors for modulating mammalian transcription. Nat Biotechnol. 2011; 29:149-153 and U.S. Pat. Nos. 8,450,471, 8,440,431 and 8,440,432, all of which are specifically incorporated by reference.

In advantageous embodiments of the invention, the methods provided herein use isolated, non-naturally occurring, recombinant or engineered DNA binding proteins that comprise TALE monomers as a part of their organizational structure that enable the targeting of nucleic acid sequences with improved efficiency and expanded specificity.

Naturally occurring TALEs or “wild type TALEs” are nucleic acid binding proteins secreted by numerous species of proteobacteria. TALE polypeptides contain a nucleic acid binding domain composed of tandem repeats of highly conserved monomer polypeptides that are predominantly 33, 34 or 35 amino acids in length and that differ from each other mainly in amino acid positions 12 and 13. In advantageous embodiments the nucleic acid is DNA. As used herein, the term “polypeptide monomers”, or “TALE monomers” will be used to refer to the highly conserved repetitive polypeptide sequences within the TALE nucleic acid binding domain and the term “repeat variable di-residues” or “RVD” will be used to refer to the highly variable amino acids at positions 12 and 13 of the polypeptide monomers. As provided throughout the disclosure, the amino acid residues of the RVD are depicted using the IUPAC single letter code for amino acids. A general representation of a TALE monomer which is comprised within the DNA binding domain is X1-11-(X12X13)-X14-33 or 34 or 35, where the subscript indicates the amino acid position and X represents any amino acid. X12X13 indicate the RVDs. In some polypeptide monomers, the variable amino acid at position 13 is missing or absent and in such polypeptide monomers, the RVD consists of a single amino acid. In such cases the RVD may be alternatively represented as X*, where X represents X12 and (*) indicates that X13 is absent. The DNA binding domain comprises several repeats of TALE monomers and this may be represented as (X1-11-(X12X13)-X14-33 or 34 or 35)z, where in an advantageous embodiment, z is at least 5 to 40. In a further advantageous embodiment, z is at least 10 to 26.

The TALE monomers have a nucleotide binding affinity that is determined by the identity of the amino acids in its RVD. For example, polypeptide monomers with an RVD of NI preferentially bind to adenine (A), polypeptide monomers with an RVD of NG preferentially bind to thymine (T), polypeptide monomers with an RVD of HD preferentially bind to cytosine (C) and polypeptide monomers with an RVD of NN preferentially bind to both adenine (A) and guanine (G). In yet another embodiment of the invention, polypeptide monomers with an RVD of IG preferentially bind to T. Thus, the number and order of the polypeptide monomer repeats in the nucleic acid binding domain of a TALE determines its nucleic acid target specificity. In still further embodiments of the invention, polypeptide monomers with an RVD of NS recognize all four base pairs and may bind to A, T, G or C. The structure and function of TALEs is further described in, for example, Moscou et al., Science 326:1501 (2009); Boch et al., Science 326:1509-1512 (2009); and Zhang et al., Nature Biotechnology 29:149-153 (2011), each of which is incorporated by reference in its entirety.

The TALE polypeptides used in methods of the invention are isolated, non-naturally occurring, recombinant or engineered nucleic acid-binding proteins that have nucleic acid or DNA binding regions containing polypeptide monomer repeats that are designed to target specific nucleic acid sequences.

As described herein, polypeptide monomers having an RVD of HN or NH preferentially bind to guanine and thereby allow the generation of TALE polypeptides with high binding specificity for guanine containing target nucleic acid sequences. In a preferred embodiment of the invention, polypeptide monomers having RVDs RN, NN, NK, SN, NH, KN, HN, NQ, HH, RG, KH, RH and SS preferentially bind to guanine. In a much more advantageous embodiment of the invention, polypeptide monomers having RVDs RN, NK, NQ, HH, KH, RH, SS and SN preferentially bind to guanine and thereby allow the generation of TALE polypeptides with high binding specificity for guanine containing target nucleic acid sequences. In an even more advantageous embodiment of the invention, polypeptide monomers having RVDs HH, KH, NH, NK, NQ, RH, RN and SS preferentially bind to guanine and thereby allow the generation of TALE polypeptides with high binding specificity for guanine containing target nucleic acid sequences. In a further advantageous embodiment, the RVDs that have high binding specificity for guanine are RN, NH RH and KH. Furthermore, polypeptide monomers having an RVD of NV preferentially bind to adenine and guanine. In more preferred embodiments of the invention, polypeptide monomers having RVDs of H*, HA, KA, N*, NA, NC, NS, RA, and S* bind to adenine, guanine, cytosine and thymine with comparable affinity.

The predetermined N-terminal to C-terminal order of the one or more polypeptide monomers of the nucleic acid or DNA binding domain determines the corresponding predetermined target nucleic acid sequence to which the TALE polypeptides will bind. As used herein the polypeptide monomers and at least one or more half polypeptide monomers are “specifically ordered to target” the genomic locus or gene of interest. In plant genomes, the natural TALE-binding sites always begin with a thymine (T), which may be specified by a cryptic signal within the non-repetitive N-terminus of the TALE polypeptide; in some cases this region may be referred to as repeat 0. In animal genomes, TALE binding sites do not necessarily have to begin with a thymine (T) and TALE polypeptides may target DNA sequences that begin with T, A, G or C. The tandem repeat of TALE monomers always ends with a half-length repeat or a stretch of sequence that may share identity with only the first 20 amino acids of a repetitive full length TALE monomer and this half repeat may be referred to as a half-monomer (FIG. 8), which is included in the term “TALE monomer”. Therefore, it follows that the length of the nucleic acid or DNA being targeted is equal to the number of full polypeptide monomers plus two.

As described in Zhang et al., Nature Biotechnology 29:149-153 (2011), TALE polypeptide binding efficiency may be increased by including amino acid sequences from the “capping regions” that are directly N-terminal or C-terminal of the DNA binding region of naturally occurring TALEs into the engineered TALEs at positions N-terminal or C-terminal of the engineered TALE DNA binding region. Thus, in certain embodiments, the TALE polypeptides described herein further comprise an N-terminal capping region and/or a C-terminal capping region.

An exemplary amino acid sequence of a N-terminal capping region is:

(SEQ ID NO: 1) M D P I R S R T P S P A R E L L S G P Q P D G V Q  P T A D R G V S P P A G G P L D G L P A R R T M S  R T R L P S P P A P S P A F S A D S F S D L L R Q  F D P S L F N T S L F D S L P P F G A H H T E A A  T G E W D E V Q S G L R A A D A P P P T M R V A V  T A A R P P R A K P A P R R R A A Q P S D A S P A  A Q V D L R T L G Y S Q Q Q Q E K I K P K V R S T  V A Q H H E A L V G H G F T H A H I V A L S Q H P  A A L G T V A V K Y Q D M I A A L P E A T H E A I  V G V G K Q W S G A R A L E A L L T V A G E L R G  P P L Q L D T G Q L L K I A K R G G V T A V E A V  H A W R N A L T G A P L N

An exemplary amino acid sequence of a C-terminal capping region is:

(SEQ ID NO: 2) R P A L E S I V A Q L S R P D P A L A A L T N D H  L V A L A C L G G R P A L D A V K K G L P H A P A  L I K R T N R R I P E R T S H R V A D H A Q V V R  V L G F F Q C H S H P A Q A F D D A M T Q F G M S  R H G L L Q L F R R V G V T E L E A R S G T L P P  A S Q R W D R I L Q A S G M K R A K P S P T S T Q  T P D Q A S L H A F A D S L E R D L D A P S P M H  E G D Q T R A S

As used herein the predetermined “N-terminus” to “C terminus” orientation of the N-terminal capping region, the DNA binding domain comprising the repeat TALE monomers and the C-terminal capping region provide structural basis for the organization of different domains in the d-TALEs or polypeptides of the invention.

The entire N-terminal and/or C-terminal capping regions are not necessary to enhance the binding activity of the DNA binding region. Therefore, in certain embodiments, fragments of the N-terminal and/or C-terminal capping regions are included in the TALE polypeptides described herein.

In certain embodiments, the TALE polypeptides described herein contain a N-terminal capping region fragment that included at least 10, 20, 30, 40, 50, 54, 60, 70, 80, 87, 90, 94, 100, 102, 110, 117, 120, 130, 140, 147, 150, 160, 170, 180, 190, 200, 210, 220, 230, 240, 250, 260 or 270 amino acids of an N-terminal capping region. In certain embodiments, the N-terminal capping region fragment amino acids are of the C-terminus (the DNA-binding region proximal end) of an N-terminal capping region. As described in Zhang et al., Nature Biotechnology 29:149-153 (2011), N-terminal capping region fragments that include the C-terminal 240 amino acids enhance binding activity equal to the full length capping region, while fragments that include the C-terminal 147 amino acids retain greater than 80% of the efficacy of the full length capping region, and fragments that include the C-terminal 117 amino acids retain greater than 50% of the activity of the full-length capping region.

In some embodiments, the TALE polypeptides described herein contain a C-terminal capping region fragment that included at least 6, 10, 20, 30, 37, 40, 50, 60, 68, 70, 80, 90, 100, 110, 120, 127, 130, 140, 150, 155, 160, 170, 180 amino acids of a C-terminal capping region. In certain embodiments, the C-terminal capping region fragment amino acids are of the N-terminus (the DNA-binding region proximal end) of a C-terminal capping region. As described in Zhang et al., Nature Biotechnology 29:149-153 (2011), C-terminal capping region fragments that include the C-terminal 68 amino acids enhance binding activity equal to the full length capping region, while fragments that include the C-terminal 20 amino acids retain greater than 50% of the efficacy of the full length capping region.

In certain embodiments, the capping regions of the TALE polypeptides described herein do not need to have identical sequences to the capping region sequences provided herein. Thus, in some embodiments, the capping region of the TALE polypeptides described herein have sequences that are at least 50%, 60%, 70%, 80%, 85%, 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99% identical or share identity to the capping region amino acid sequences provided herein. Sequence identity is related to sequence homology. Homology comparisons may be conducted by eye, or more usually, with the aid of readily available sequence comparison programs. These commercially available computer programs may calculate percent (%) homology between two or more sequences and may also calculate the sequence identity shared by two or more amino acid or nucleic acid sequences. In some preferred embodiments, the capping region of the TALE polypeptides described herein have sequences that are at least 95% identical or share identity to the capping region amino acid sequences provided herein.

Sequence homologies may be generated by any of a number of computer programs known in the art, which include but are not limited to BLAST or FASTA. Suitable computer program for carrying out alignments like the GCG Wisconsin Bestfit package may also be used. Once the software has produced an optimal alignment, it is possible to calculate % homology, preferably % sequence identity. The software typically does this as part of the sequence comparison and generates a numerical result.

In advantageous embodiments described herein, the TALE polypeptides of the invention include a nucleic acid binding domain linked to the one or more effector domains. The terms “effector domain” or “regulatory and functional domain” refer to a polypeptide sequence that has an activity other than binding to the nucleic acid sequence recognized by the nucleic acid binding domain. By combining a nucleic acid binding domain with one or more effector domains, the polypeptides of the invention may be used to target the one or more functions or activities mediated by the effector domain to a particular target DNA sequence to which the nucleic acid binding domain specifically binds.

In some embodiments of the TALE polypeptides described herein, the activity mediated by the effector domain is a biological activity. For example, in some embodiments the effector domain is a transcriptional inhibitor (i.e., a repressor domain), such as an mSin interaction domain (SID). SID4X domain or a Kruppel-associated box (KRAB) or fragments of the KRAB domain. In some embodiments the effector domain is an enhancer of transcription (i.e. an activation domain), such as the VP16, VP64 or p65 activation domain. In some embodiments, the nucleic acid binding is linked, for example, with an effector domain that includes but is not limited to a transposase, integrase, recombinase, resolvase, invertase, protease, DNA methyltransferase, DNA demethylase, histone acetylase, histone deacetylase, nuclease, transcriptional repressor, transcriptional activator, transcription factor recruiting, protein nuclear-localization signal or cellular uptake signal.

In some embodiments, the effector domain is a protein domain which exhibits activities which include but are not limited to transposase activity, integrase activity, recombinase activity, resolvase activity, invertase activity, protease activity, DNA methyltransferase activity, DNA demethylase activity, histone acetylase activity, histone deacetylase activity, nuclease activity, nuclear-localization signaling activity, transcriptional repressor activity, transcriptional activator activity, transcription factor recruiting activity, or cellular uptake signaling activity. Other preferred embodiments of the invention may include any combination the activities described herein.

ZN-Finger Nucleases

Other preferred tools for genome editing for use in the context of this invention include zinc finger systems and TALE systems. One type of programmable DNA-binding domain is provided by artificial zinc-finger (ZF) technology, which involves arrays of ZF modules to target new DNA-binding sites in the genome. Each finger module in a ZF array targets three DNA bases. A customized array of individual zinc finger domains is assembled into a ZF protein (ZFP).

ZFPs can comprise a functional domain. The first synthetic zinc finger nucleases (ZFNs) were developed by fusing a ZF protein to the catalytic domain of the Type IIS restriction enzyme FokI. (Kim, Y. G. et al., 1994, Chimeric restriction endonuclease, Proc. Natl. Acad. Sci. U.S.A. 91, 883-887; Kim, Y. G. et al., 1996, Hybrid restriction enzymes: zinc finger fusions to Fok I cleavage domain. Proc. Natl. Acad. Sci. U.S.A. 93, 1156-1160). Increased cleavage specificity can be attained with decreased off target activity by use of paired ZFN heterodimers, each targeting different nucleotide sequences separated by a short spacer. (Doyon, Y. et al., 2011, Enhancing zinc-finger-nuclease activity with improved obligate heterodimeric architectures. Nat. Methods 8, 74-79). ZFPs can also be designed as transcription activators and repressors and have been used to target many genes in a wide variety of organisms. Exemplary methods of genome editing using ZFNs can be found for example in U.S. Pat. Nos. 6,534,261, 6,607,882, 6,746,838, 6,794,136, 6,824,978, 6,866,997, 6,933,113, 6,979,539, 7,013,219, 7,030,215, 7,220,719, 7,241,573, 7,241,574, 7,585,849, 7,595,376, 6,903,185, and 6,479,626, all of which are specifically incorporated by reference.

Meganucleases

As disclosed herein editing can be made by way of meganucleases, which are endodeoxyribonucleases characterized by a large recognition site (double-stranded DNA sequences of 12 to 40 base pairs). Exemplary method for using meganucleases can be found in U.S. Pat. Nos. 8,163,514; 8,133,697; 8,021,867; 8,119,361; 8,119,381; 8,124,369; and 8,129,134, which are specifically incorporated by reference.

Pharmaceuticals

Another aspect of the invention provides a composition, pharmaceutical composition or vaccine comprising the intestinal epithelial cells, intestinal epithelial stem cells, or intestinal immune cells (preferably intestinal epithelial cells) or populations thereof as taught herein.

A “pharmaceutical composition” refers to a composition that usually contains an excipient, such as a pharmaceutically acceptable carrier that is conventional in the art and that is suitable for administration to cells or to a subject.

The term “pharmaceutically acceptable” as used throughout this specification is consistent with the art and means compatible with the other ingredients of a pharmaceutical composition and not deleterious to the recipient thereof.

As used herein, “carrier” or “excipient” includes any and all solvents, diluents, buffers (such as, e.g., neutral buffered saline or phosphate buffered saline), solubilisers, colloids, dispersion media, vehicles, fillers, chelating agents (such as, e.g., EDTA or glutathione), amino acids (such as, e.g., glycine), proteins, disintegrants, binders, lubricants, wetting agents, emulsifiers, sweeteners, colorants, flavourings, aromatisers, thickeners, agents for achieving a depot effect, coatings, antifungal agents, preservatives, stabilisers, antioxidants, tonicity controlling agents, absorption delaying agents, and the like. The use of such media and agents for pharmaceutical active components is well known in the art. Such materials should be non-toxic and should not interfere with the activity of the cells or active components.

The precise nature of the carrier or excipient or other material will depend on the route of administration. For example, the composition may be in the form of a parenterally acceptable aqueous solution, which is pyrogen-free and has suitable pH, isotonicity and stability. For general principles in medicinal formulation, the reader is referred to Cell Therapy: Stem Cell Transplantation, Gene Therapy, and Cellular Immunotherapy, by G. Morstyn & W. Sheridan eds., Cambridge University Press, 1996; and Hematopoietic Stem Cell Therapy, E. D. Ball, J. Lister & P. Law, Churchill Livingstone, 2000.

The pharmaceutical composition can be applied parenterally, rectally, orally or topically. Preferably, the pharmaceutical composition may be used for intravenous, intramuscular, subcutaneous, peritoneal, peridural, rectal, nasal, pulmonary, mucosal, or oral application. In a preferred embodiment, the pharmaceutical composition according to the invention is intended to be used as an infuse. The skilled person will understand that compositions which are to be administered orally or topically will usually not comprise cells, although it may be envisioned for oral compositions to also comprise cells, for example when gastro-intestinal tract indications are treated. Each of the cells or active components (e.g., modulants, immunomodulants, antigens) as discussed herein may be administered by the same route or may be administered by a different route. By means of example, and without limitation, cells may be administered parenterally and other active components may be administered orally.

Liquid pharmaceutical compositions may generally include a liquid carrier such as water or a pharmaceutically acceptable aqueous solution. For example, physiological saline solution, tissue or cell culture media, dextrose or other saccharide solution or glycols such as ethylene glycol, propylene glycol or polyethylene glycol may be included.

The composition may include one or more cell protective molecules, cell regenerative molecules, growth factors, anti-apoptotic factors or factors that regulate gene expression in the cells. Such substances may render the cells independent of their environment.

Such pharmaceutical compositions may contain further components ensuring the viability of the cells therein. For example, the compositions may comprise a suitable buffer system (e.g., phosphate or carbonate buffer system) to achieve desirable pH, more usually near neutral pH, and may comprise sufficient salt to ensure isoosmotic conditions for the cells to prevent osmotic stress. For example, suitable solution for these purposes may be phosphate-buffered saline (PBS), sodium chloride solution, Ringer's Injection or Lactated Ringer's Injection, as known in the art. Further, the composition may comprise a carrier protein, e.g., albumin (e.g., bovine or human albumin), which may increase the viability of the cells.

Further suitably pharmaceutically acceptable carriers or additives are well known to those skilled in the art and for instance may be selected from proteins such as collagen or gelatine, carbohydrates such as starch, polysaccharides, sugars (dextrose, glucose and sucrose), cellulose derivatives like sodium or calcium carboxymethylcellulose, hydroxypropyl cellulose or hydroxypropylmethyl cellulose, pregeletanized starches, pectin agar, carrageenan, clays, hydrophilic gums (acacia gum, guar gum, arabic gum and xanthan gum), alginic acid, alginates, hyaluronic acid, polyglycolic and polylactic acid, dextran, pectins, synthetic polymers such as water-soluble acrylic polymer or polyvinylpyrrolidone, proteoglycans, calcium phosphate and the like.

If desired, cell preparation can be administered on a support, scaffold, matrix or material to provide improved tissue regeneration. For example, the material can be a granular ceramic, or a biopolymer such as gelatine, collagen, or fibrinogen. Porous matrices can be synthesized according to standard techniques (e.g., Mikos et al., Biomaterials 14: 323, 1993; Mikos et al., Polymer 35:1068, 1994; Cook et al., J. Biomed. Mater. Res. 35:513, 1997). Such support, scaffold, matrix or material may be biodegradable or non-biodegradable. Hence, the cells may be transferred to and/or cultured on suitable substrate, such as porous or non-porous substrate, to provide for implants.

For example, cells that have proliferated, or that are being differentiated in culture dishes, can be transferred onto three-dimensional solid supports in order to cause them to multiply and/or continue the differentiation process by incubating the solid support in a liquid nutrient medium of the invention, if necessary. Cells can be transferred onto a three-dimensional solid support, e.g. by impregnating the support with a liquid suspension containing the cells. The impregnated supports obtained in this way can be implanted in a human subject. Such impregnated supports can also be re-cultured by immersing them in a liquid culture medium, prior to being finally implanted. The three-dimensional solid support needs to be biocompatible so as to enable it to be implanted in a human. It may be biodegradable or non-biodegradable.

The cells or cell populations can be administered in a manner that permits them to survive, grow, propagate and/or differentiate towards desired cell types (e.g. differentiation) or cell states. The cells or cell populations may be grafted to or may migrate to and engraft within the intended organ.

In certain embodiments, a pharmaceutical cell preparation as taught herein may be administered in a form of liquid composition. In embodiments, the cells or pharmaceutical composition comprising such can be administered systemically, topically, within an organ or at a site of organ dysfunction or lesion.

Preferably, the pharmaceutical compositions may comprise a therapeutically effective amount of the specified intestinal epithelial cells, intestinal epithelial stem cells, or intestinal immune cells (preferably intestinal epithelial cells) and/or other active components. The term “therapeutically effective amount” refers to an amount which can elicit a biological or medicinal response in a tissue, system, animal or human that is being sought by a researcher, veterinarian, medical doctor or other clinician, and in particular can prevent or alleviate one or more of the local or systemic symptoms or features of a disease or condition being treated.

A further aspect of the invention provides a population of the intestinal epithelial cells, intestinal epithelial stem cells, or intestinal immune cells (preferably intestinal epithelial cells) as taught herein. The terms “cell population” or “population” denote a set of cells having characteristics in common. The characteristics may include in particular the one or more marker(s) or gene or gene product signature(s) as taught herein. The intestinal epithelial cells, intestinal epithelial stem cells, or intestinal immune cells (preferably intestinal epithelial cells) cells as taught herein may be comprised in a cell population. By means of example, the specified cells may constitute at least 40% (by number) of all cells of the cell population, for example, at least 45%, preferably at least 50%, at least 55%, more preferably at least 60%, at least 65%, still more preferably at least 70%, at least 75%, even more preferably at least 80%, at least 85%, and yet more preferably at least 90%, at least 95%, at least 96%, at least 97%, at least 98%, at least 99%, or even 100% of all cells of the cell population.

The isolated intestinal epithelial cells, intestinal epithelial stem cells, or intestinal immune cells (preferably intestinal epithelial cells) of populations thereof as disclosed throughout this specification may be suitably cultured or cultivated in vitro. The term “in vitro” generally denotes outside, or external to, a body, e.g., an animal or human body. The term encompasses “ex vivo”. The terms “culturing” or “cell culture” are common in the art and broadly refer to maintenance of cells and potentially expansion (proliferation, propagation) of cells in vitro. Typically, animal cells, such as mammalian cells, such as human cells, are cultured by exposing them to (i.e., contacting them with) a suitable cell culture medium in a vessel or container adequate for the purpose (e.g., a 96-, 24-, or 6-well plate, a T-25, T-75, T-150 or T-225 flask, or a cell factory), at art-known conditions conducive to in vitro cell culture, such as temperature of 37° C., 5% v/v CO₂ and >95% humidity.

The term “medium” as used herein broadly encompasses any cell culture medium conducive to maintenance of cells, preferably conducive to proliferation of cells. Typically, the medium will be a liquid culture medium, which facilitates easy manipulation (e.g., decantation, pipetting, centrifugation, filtration, and such) thereof.

Differentiation

A relatively more specialised cell may differ from an unspecialised or relatively less specialised cell in one or more demonstrable phenotypic characteristics, such as, for example, the presence, absence or level of expression of particular cellular components or products, e.g., RNA, proteins or other substances, activity of certain biochemical pathways, morphological appearance, proliferation capacity and/or kinetics, differentiation potential and/or response to differentiation signals, electrophysiological behaviour, etc., wherein such characteristics signify the progression of the relatively more specialised cell further along the developmental pathway. Non-limiting examples of differentiation may include, e.g., the change of a pluripotent stem cell into a given type of multipotent progenitor or stem cell, the change of a multipotent progenitor or stem cell into a given type of unipotent progenitor or stem cell, or the change of a unipotent progenitor or stem cell to more specialised cell types or to terminally specialised cells within a given cell lineage.

The terms “diagnosis” and “monitoring” are commonplace and well-understood in medical practice. By means of further explanation and without limitation the term “diagnosis” generally refers to the process or act of recognising, deciding on or concluding on a disease or condition in a subject on the basis of symptoms and signs and/or from results of various diagnostic procedures (such as, for example, from knowing the presence, absence and/or quantity of one or more biomarkers characteristic of the diagnosed disease or condition).

The term “monitoring” generally refers to the follow-up of a disease or a condition in a subject for any changes which may occur over time.

The terms “prognosing” or “prognosis” generally refer to an anticipation on the progression of a disease or condition and the prospect (e.g., the probability, duration, and/or extent) of recovery. A good prognosis of the diseases or conditions taught herein may generally encompass anticipation of a satisfactory partial or complete recovery from the diseases or conditions, preferably within an acceptable time period. A good prognosis of such may more commonly encompass anticipation of not further worsening or aggravating of such, preferably within a given time period. A poor prognosis of the diseases or conditions as taught herein may generally encompass anticipation of a substandard recovery and/or unsatisfactorily slow recovery, or to substantially no recovery or even further worsening of such.

The terms also encompass prediction of a disease. The terms “predicting” or “prediction” generally refer to an advance declaration, indication or foretelling of a disease or condition in a subject not (yet) having the disease or condition. For example, a prediction of a disease or condition in a subject may indicate a probability, chance or risk that the subject will develop the disease or condition, for example within a certain time period or by a certain age. The probability, chance or risk may be indicated inter alia as an absolute value, range or statistics, or may be indicated relative to a suitable control subject or subject population (such as, e.g., relative to a general, normal or healthy subject or subject population). Hence, the probability, chance or risk that a subject will develop a disease or condition may be advantageously indicated as increased or decreased, or as fold-increased or fold-decreased relative to a suitable control subject or subject population. As used herein, the term “prediction” of the conditions or diseases as taught herein in a subject may also particularly mean that the subject has a ‘positive’ prediction of such, i.e., that the subject is at risk of having such (e.g., the risk is significantly increased vis-à-vis a control subject or subject population). The term “prediction of no” diseases or conditions as taught herein as described herein in a subject may particularly mean that the subject has a ‘negative’ prediction of such, i.e., that the subject's risk of having such is not significantly increased vis-à-vis a control subject or subject population.

As used throughout this specification, the terms “treat”, “treating” and “treatment” refer to the alleviation or measurable lessening of one or more symptoms or measurable markers of a pathological condition such as a disease or disorder. Measurable lessening includes any statistically significant decline in a measurable marker or symptom. Generally, the terms encompass both curative treatments and treatments directed to reduce symptoms and/or slow progression of the disease. The terms encompass both the therapeutic treatment of an already developed pathological condition, as well as prophylactic or preventative measures, wherein the aim is to prevent or lessen the chances of incidence of a pathological condition. In certain embodiments, the terms may relate to therapeutic treatments. In certain other embodiments, the terms may relate to preventative treatments. Treatment of a chronic pathological condition during the period of remission may also be deemed to constitute a therapeutic treatment. The term may encompass ex vivo or in vivo treatments as appropriate in the context of the present invention.

As used throughout this specification, the terms “prevent”, “preventing” and “prevention” refer to the avoidance or delay in manifestation of one or more symptoms or measurable markers of a pathological condition, such as a disease or disorder. A delay in the manifestation of a symptom or marker is a delay relative to the time at which such symptom or marker manifests in a control or untreated subject with a similar likelihood or susceptibility of developing the pathological condition. The terms “prevent”, “preventing” and “prevention” include not only the avoidance or prevention of a symptom or marker of the pathological condition, but also a reduced severity or degree of any one of the symptoms or markers of the pathological condition, relative to those symptoms or markers in a control or non-treated individual with a similar likelihood or susceptibility of developing the pathological condition, or relative to symptoms or markers likely to arise based on historical or statistical measures of populations affected by the disease or disorder. By “reduced severity” is meant at least a 10% reduction in the severity or degree of a symptom or measurable marker relative to a control or reference, e.g., at least 15%, 20%, 30%, 40%, 50%, 60%, 70%, 80%, 90%, 95%, 99% or even 100% (i.e., no symptoms or measurable markers).

The terms “disease” or “disorder” are used interchangeably throughout this specification, and refer to any alternation in state of the body or of some of the organs, interrupting or disturbing the performance of the functions and/or causing symptoms such as discomfort, dysfunction, distress, or even death to the person afflicted or those in contact with a person. A disease or disorder can also be related to a distemper, ailing, ailment, malady, disorder, sickness, illness, complaint, indisposition, or affliction.

In certain embodiments, the pathological condition may be an infection, inflammation, proliferative disease, autoimmune disease, or allergy.

The term “infection” as used herein refers to presence of an infective agent, such as a pathogen, e.g., a microorganism, in or on a subject, which, if its presence or growth were inhibited, would result in a benefit to the subject. Hence, the term refers to the state produced by the establishment, more particularly invasion and multiplication, of an infective agent, such as a pathogen, e.g., a microorganism, in or on a suitable host. An infection may produce tissue injury and progress to overt disease through a variety of cellular and toxic mechanisms.

The term “inflammation” generally refers to a response in vasculated tissues to cellular or tissue injury usually caused by physical, chemical and/or biological agents, that is marked in the acute form by the classical sequences of pain, heat, redness, swelling, and loss of function, and serves as a mechanism initiating the elimination, dilution or walling-off of noxious agents and/or of damaged tissue. Inflammation histologically involves a complex series of events, including dilation of the arterioles, capillaries, and venules with increased permeability and blood flow, exudation of fluids including plasma proteins, and leukocyte migration into the inflammatory focus.

Further, the term encompasses inflammation caused by extraneous physical or chemical injury or by biological agents, e.g., viruses, bacteria, fungi, protozoan or metazoan parasite infections, as well as inflammation which is seemingly unprovoked, e.g., which occurs in the absence of demonstrable injury or infection, inflammation responses to self-antigens (auto-immune inflammation), inflammation responses to engrafted xenogeneic or allogeneic cells, tissues or organs, inflammation responses to allergens, etc. The term covers both acute inflammation and chronic inflammation. Also, the term includes both local or localised inflammation, as well as systemic inflammation, i.e., where one or more inflammatory processes are not confined to a particular tissue but occur generally in the endothelium and/or other organ systems.

Systemic inflammatory conditions may particularly encompass systemic inflammatory response syndrome (SIRS) or sepsis. “SIRS” is a systemic inflammatory response syndrome with no signs of infection. It can be characterised by the presence of at least two of the four following clinical criteria: fever or hypothermia (temperature of 38.0° C.) or more, or temperature of 36.0° C. or less); tachycardia (at least 90 beats per minute); tachypnea (at least 20 breaths per minute or PaCO₂ less than 4.3 kPa (32.0 mm Hg) or the need for mechanical ventilation); and an altered white blood cell (WBC) count of 12×10⁶ cells/mL or more, or an altered WBC count of 4×10⁶ cells/mL or less, or the presence of more than 10% band forms. “Sepsis” can generally be defined as SIRS with a documented infection, such as for example a bacterial infection. Infection can be diagnosed by standard textbook criteria or, in case of uncertainty, by an infectious disease specialist. Bacteraemia is defined as sepsis where bacteria can be cultured from blood. Sepsis may be characterised or staged as mild sepsis, severe sepsis (sepsis with acute organ dysfunction), septic shock (sepsis with refractory arterial hypotension), organ failure, multiple organ dysfunction syndrome and death.

The term “proliferative disease” generally refers to any disease or disorder characterised by neoplastic cell growth and proliferation, whether benign, pre-malignant, or malignant. The term proliferative disease generally includes all transformed cells and tissues and all cancerous cells and tissues. Proliferative diseases or disorders include, but are not limited to abnormal cell growth, benign tumours, premalignant or precancerous lesions, malignant tumors, and cancer.

The terms “tumor” or “tumor tissue” refer to an abnormal mass of tissue resulting from excessive cell division. A tumor or tumor tissue comprises “tumor cells” which are neoplastic cells with abnormal growth properties and no useful bodily function. Tumors, tumor tissue and tumor cells may be benign, pre-malignant or malignant, or may represent a lesion without any cancerous potential. A tumor or tumor tissue may also comprise “tumor-associated non-tumor cells”, e.g., vascular cells which form blood vessels to supply the tumor or tumor tissue. Non-tumor cells may be induced to replicate and develop by tumor cells, for example, the induction of angiogenesis in a tumor or tumor tissue.

The term “cancer” refers to a malignant neoplasm characterised by deregulated or unregulated cell growth. The term “cancer” includes primary malignant cells or tumors (e.g., those whose cells have not migrated to sites in the subject's body other than the site of the original malignancy or tumor) and secondary malignant cells or tumors (e.g., those arising from metastasis, the migration of malignant cells or tumor cells to secondary sites that are different from the site of the original tumor. The term “metastatic” or “metastasis” generally refers to the spread of a cancer from one organ or tissue to another non-adjacent organ or tissue. The occurrence of the proliferative disease in the other non-adjacent organ or tissue is referred to as metastasis.

As used throughout the present specification, the terms “autoimmune disease” or “autoimmune disorder” used interchangeably refer to a diseases or disorders caused by an immune response against a self-tissue or tissue component (self-antigen) and include a self-antibody response and/or cell-mediated response. The terms encompass organ-specific autoimmune diseases, in which an autoimmune response is directed against a single tissue, as well as non-organ specific autoimmune diseases, in which an autoimmune response is directed against a component present in two or more, several or many organs throughout the body.

Non-limiting examples of autoimmune diseases include but are not limited to acute disseminated encephalomyelitis (ADEM); Addison's disease; ankylosing spondylitis; antiphospholipid antibody syndrome (APS); aplastic anemia; autoimmune gastritis; autoimmune hepatitis; autoimmune thrombocytopenia; Behget's disease; coeliac disease; dermatomyositis; diabetes mellitus type I; Goodpasture's syndrome; Graves' disease; Guillain-Barré syndrome (GBS); Hashimoto's disease; idiopathic thrombocytopenic purpura; inflammatory bowel disease (IBD) including Crohn's disease and ulcerative colitis; mixed connective tissue disease; multiple sclerosis (MS); myasthenia gravis; opsoclonus myoclonus syndrome (OMS); optic neuritis; Ord's thyroiditis; pemphigus; pernicious anaemia; polyarteritis nodosa; polymyositis; primary biliary cirrhosis; primary myoxedema; psoriasis; rheumatic fever; rheumatoid arthritis; Reiter's syndrome; scleroderma; Sjögren's syndrome; systemic lupus erythematosus; Takayasu's arteritis; temporal arteritis; vitiligo; warm autoimmune hemolytic anemia; or Wegener's granulomatosis.

“Activation” generally refers to the state of a cell, such as preferably T cell, following sufficient cell surface moiety ligation (e.g., interaction between the T cell receptor on the surface of a T cell (such as naturally-occurring TCR or genetically engineered TCR, e.g., chimeric antigen receptor, CAR) and MHC-bound antigen peptide presented on the surface of the immune cell as taught herein) to induce a noticeable biochemical or morphological change of the cell, such as preferably T cell. In particular, “activation” may refer to the state of a T cell that has been sufficiently stimulated to induce detectable cellular proliferation of the T cell. Activation can also encompass induced cytokine production, and detectable T cell effector functions, e.g., regulatory or cytolytic effector functions. The T cells and immune cells may be may be suitably contacted by admixing the T cells and immune cells in an aqueous composition, e.g., in a culture medium, in sufficient numbers and for a sufficient duration of time to produce the desired T cell activation.

The terms “increased” or “increase” or “upregulated” or “upregulate” as used herein generally mean an increase by a statically significant amount. For avoidance of doubt, “increased” means a statistically significant increase of at least 10% as compared to a reference level, including an increase of at least 20%, at least 30%, at least 40%, at least 50%, at least 60%, at least 70%, at least 80%, at least 90%, at least 100% or more, including, for example at least 2-fold, at least 3-fold, at least 4-fold, at least 5-fold, at least 10-fold increase or greater as compared to a reference level, as that term is defined herein.

The term “reduced” or “reduce” or “decrease” or “decreased” or “downregulate” or “downregulated” as used herein generally means a decrease by a statistically significant amount relative to a reference. For avoidance of doubt, “reduced” means statistically significant decrease of at least 10% as compared to a reference level, for example a decrease by at least 20%, at least 30%, at least 40%, at least t 50%, or least 60%, or least 70%, or least 80%, at least 90% or more, up to and including a 100% decrease (i.e., absent level as compared to a reference sample), or any decrease between 10-100% as compared to a reference level, as that term is defined herein. The term “abolish” or “abolished” may in particular refer to a decrease by 100%, i.e., absent level as compared to a reference sample.

Any one or more of the several successive molecular mechanisms involved in the expression of a given gene or polypeptide may be targeted by the intestinal epithelial cells, intestinal epithelial stem cells, or intestinal immune cells (preferably intestinal epithelial cells) cell modification as intended herein. Without limitation, these may include targeting the gene sequence (e.g., targeting the polypeptide-encoding, non-coding and/or regulatory portions of the gene sequence), the transcription of the gene into RNA, the polyadenylation and where applicable splicing and/or other post-transcriptional modifications of the RNA into mRNA, the localization of the mRNA into cell cytoplasm, where applicable other post-transcriptional modifications of the mRNA, the translation of the mRNA into a polypeptide chain, where applicable post-translational modifications of the polypeptide, and/or folding of the polypeptide chain into the mature conformation of the polypeptide. For compartmentalized polypeptides, such as secreted polypeptides and transmembrane polypeptides, this may further include targeting trafficking of the polypeptides, i.e., the cellular mechanism by which polypeptides are transported to the appropriate sub-cellular compartment or organelle, membrane, e.g. the plasma membrane, or outside the cell. Functional genomics can be used to modify cells for therapeutic purposes, and identify networks and pathways. For example, Graham et al (“Functional genomics identifies negative regulatory nodes controlling phagocyte oxidative burst,” Nature Communications 6, Article number: 7838 (2015)) describes functional genetic screens to identify the phagocytic oxidative burst. With the rapid advancement of genomic technology, it is now possible to associate genetic variation with phenotypes of intestinal epithelial cells, intestinal epithelial stem cells, or intestinal immune cells (preferably intestinal epithelial cells) at the population level. In particular, genome-wide association studies (GWAS) have implicated genetic loci associated with risk for IBD and allowed for inference of new biological processes that contribute to disease. These studies highlight innate defense mechanisms such as antibacterial autophagy, superoxide generation during oxidative burst and reactive nitrogen species produced by iNOS. However, GWAS requires functional analysis to unlock new insights. For example, many risk loci are densely populated with coding genes, which complicates identification of causal genes. Even when fine mapping clearly identifies key genes, a majority have poorly defined functions in host immunity. Moreover, any given gene may have multiple functions depending on the cell type in which it is expressed as well as environmental cues. Such context-specific functions of regulatory genes are largely unexplored. Thus, human genetics offers an opportunity to leverage insight from large amounts of genetic variation within healthy and patient populations to interrogate mechanisms of immunity. Irrespective of their putative roles in IBD pathology, genes within risk loci are likely to be highly enriched for genes controlling signaling pathways.

The invention is further described in the following examples, which do not limit the scope of the invention described in the claims.

EXAMPLES Example 1—Map of the Cellular and Molecular Composition in the Healthy and Inflamed Gut

Applicants have generated a foundational resource in the healthy and inflamed gut for: (1) Cell composition (i.e., changes in proportions of different cell types/states), (2) Cell intrinsic states (i.e., changes in gene expression within a cell type), (3) Cell-cell interactions (i.e., changes in cell-cell interaction mechanisms), and (4) the relevant cell types for each gene (e.g., GWAS genes).

GWAS gene→cell type→cell state→cell interaction→disease

Applicants used single cell RNA-seq of colonoscopy samples from healthy individuals and UC patients to generate the cell atlas. The samples were obtained from 10 healthy individuals (37,435 non-inflamed cells were initially analyzed), 10 UC patients (17,400 cells (10,688 uninflamed; 6,712 inflamed) were initially analyzed). Three additional samples were analyzed. In total 117,819 cells were analyzed (49,765 epithelial, 11,556 stromal, 56,498 immune). The samples were small biopsies containing about <80,000 cells. The biopsies were fresh and dislocation and processing were performed by applicants. A subset of greater than 50,000 cells are presented on some plots herein.

FIG. 1 shows that initial clustering analysis partitioned cells by patient in the UC samples and by cell type in the healthy samples. This result was similar as in Tirosh, et al. (Dissecting the multicellular ecosystem of metastatic melanoma by single-cell RNA-seq. Science 2016, 352, 189-196) where malignant cells partitioned by patient and non-malignant cells partitioned by cell type. Applicants used computational modeling to address the batch effects and partition the cells by cell type (FIG. 2).

FIGS. 3 and 4 show that the atlas uncovers almost all cell types and subtypes in the colon. Applicants identified the following cell types and subtypes in the colon: Plasma B cells, Class switching B cells, Follicular B cells, T cells, Macrophages, Dendritic cells, Mast cells, Cycling monocytes, Tolerogenic DCs, Neutrophils, Activated CD4 cells loFos, Activated CD4 cells hiFos, CD8 IELs, CD8 LP cells, Tregs, Memory T cells, NK cells, Cycling CD8 cells, Microvascular cells, Post-capillary venules, Vitamin metabolizing, Endothelial pericytes, Enterocytes, Tuft cells, Goblet 2, Absorptive TA 1, Secretory TA, Absorptive TA 2, Cycling TA, Goblet 1, Stem cells, Enteroendocrine, Glial cells, Inflammatory fibroblasts, Fibroblast pericytes, Myofibroblasts, Villus fibroblasts, Crypt fibroblasts (hiFos) and Crypt fibroblasts (loFos). Applicants identified markers specific for each cell type. Table 1 A-D shows the top 250 genes expressed in each cell type.

TABLE 1A Plasma_B_cells Class_switching_B_cells Follicular_B_cells Microvascular_cells Post-capillary_venules HERPUD1 IGLL5 CD79A PRSS23 DARC IGJ IGJ MS4A1 RGCC NPC2 SSR4 TMSB10 CD79B PLVAP CLDN5 SEC11C CFL1 VPREB3 VWA1 CPE XBP1 TMSB4X TCL1A PASK MADCAM1 MZB1 PFN1 FCRLA GNG11 CLU FKBP11 MYL6 CD37 CA4 DUSP23 DERL3 FTH1 CD19 CD36 JAM2 SPCS2 GAPDH SMIM14 CD320 PLVAP TNFRSF17 ACTB CST3 VWF LY6E CD79A IGLL1 CD63 ENG ECSCR SSR3 TNFRSF17 LTB RAMP2 SDCBP UBE2J1 CD79A LIMD2 SLC9A3R2 TSPAN7 SPCS1 DERL3 CD22 ESAM EGFL7 DNAJB9 MT-CO1 BLK CRIP2 VWF EAF2 MZB1 LGALS3 GSN GNG11 FKBP2 SERF2 PTPRCAP SPARCL1 RAMP2 MANF AL928768.3 AL928768.3 FKBP1A APLNR PRDX4 ACTG1 HLA-DQA1 TMEM204 RAMP3 SDF2L1 RPL28 CD53 ITM2B ITM2B SERP1 RPS24 BANK1 RBP5 CTNNAL1 AL928768.3 MT-CO3 RHOH TM4SF18 IGFBP4 SPCS3 ATP5E S100A6 RAMP3 NNMT CYBA COX4I1 GPR18 EGFL7 HLA-E WT1-AS HLA-A CORO1A HSPG2 GIMAP7 CRELD2 PPAPDC1B BCAS4 CCDC85B GPR126 VIMP GNG7 CXCR5 ECSCR ICAM1 SEC61B UBA52 CD74 TMEM88 HHEX PDIA6 ICAM3 SERPINA9 SDPR GIMAP4 HSP90B1 UQCR11 LRMP VAMP5 TNFSF10 GNG7 RPS12 FCGRT BCAM LINC01013 PPAPDC1B SSR4 EAF2 CAV1 AC011526.1 CD27 S100A6 RGS13 MGP CLEC14A FAM46C PPDPF CXCR4 EMCN IGFBP7 PDIA4 RPL31 POU2AF1 ELTD1 NPDC1 ISG20 CHCHD2 SMARCB1 PLAT NCOA7 PABPC4 BTF3 CD52 KDR CAV1 TRAM1 SRP14 SPIB CLEC14A LMO2 ANKRD37 CD27 MGST3 HLA-E SNCG RPL36AL TOMM7 BLNK IGFBP7 CTGF C19orf10 PFDN5 HLA-DRA FLT1 TM4SF1 CCR10 MYL12B CD72 PODXL FAM213A IGLL5 YBX1 POU2F2 SEPW1 SPARCL1 HSPA5 EAF2 ACTR3 IGFBP4 CRIP2 ACTB UBE2J1 FCRL2 HTRA1 ITM2A LMAN2 SRGN HMGN1 SPARC FAM167B MEI1 RPL30 CD40 CAV2 FKBP1A DUSP5 EIF3K ARPC2 SLC14A1 ESAM SELK NDUFA11 GGA2 AC011526.1 IFITM3 UBC CYTIP EZR SH3BP5 TMEM100 FCRL5 RPL23 HERPUD1 FAM167B CCL14 CST3 TRAM1 NCF1 FAM213A BCAM TXNDC11 ATP5G2 IRF8 SNCG GIMAP1 UAP1 FAM46C HLA-DPA1 GIMAP7 CD34 PIM2 TCEB2 HLA-DQB1 CDC37 IFI27 CFL1 PTMA HLA-DPB1 IFITM3 TGFBR2 SPAG4 ERLEC1 LAPTM5 RP11-536018.2 CYBA YPEL5 SH3BGRL3 UBE2J1 PPAP2A RBP5 PFN1 EDF1 HLA-DOB TSC22D1 CYYR1 S100A6 HM13 FCER2 IFITM2 ZNF385D TPD52 RPS7 C12orf75 ICAM2 NRN1 CHPF KDELR1 SWAP70 PTRF HLA-DRA RP11-90F5.1 ARHGDIB HMCES EHD4 ADIRF HSPA1B FKBP11 BTG1 NQO1 CD320 POU2AF1 PABPC4 P2RX5 CLDN5 CD59 JUN SPCS3 LY86 CD59 SRPX BTG2 RPL38 CYTIP COL4A1 ENG TXNDC15 COX6B1 METAP2 PPAP2B CFI TSC22D3 ALDOA CD180 HLA-C HLA-A TMEM258 RPS11 AICDA CXorf36 HSPB1 TMED10 CLIC1 CD9 NPDC1 HLA-DPB1 MCL1 TPI1 LY9 ARHGAP29 PIM3 TMSB10 TXNDC15 HLA-DRB1 ANGPT2 HLA-DRB5 TPST2 RPL10A ANXA2 HSPB1 SEPW1 ACTG1 CHST12 ISG20 CD34 SDPR NR4A1 NDUFA13 SEPW1 TM4SF1 ENPP2 S100A10 TRMT112 ARHGDIB APP NOSTRIN TNFRSF18 DPP7 HMGA1 BAALC DNAJA1 ERLEC1 IFNAR2 TCEA1 C16orf80 PTRF NUCB2 RPL11 POLD4 EFNA1 KCTD12 TMSB4X MYL12A CD83 ACVRL1 IFITM2 RPN2 RPSA BASP1 LXN HLA-DRB1 SUB1 RPL26 STAG3 IGFBP3 MYCT1 PNOC ISG20 S100A11 CYYR1 GIMAP5 SELM ATP6V1G1 SNX29P2 MYL12A CCDC85B SLAMF7 RPL27 TPD52 MGLL CNN3 IFNAR2 POU2AF1 IFI27 HLA-A LMCD1 DDOST ALG5 ARPC3 HLA-DRA KANK3 MYL12B PSMA7 HTR3A STOM CD74 TNFRSF13B RPL24 GCSAM EGLN3 HLA-DPA1 FGF23 SLC25A3 PNOC ROBO4 HLA-C LMAN1 SEC62 E2F5 SPTBN1 CDH5 ANKRD28 CNPY2 CD27 ABI3 ADM5 CD38 BST2 RAC2 HLX NFKBIA ICAM3 TMEM230 AC023590.1 RASIP1 SPARC GAPDH RPL37 STX7 HLA-B PALMD DNAJB11 CD63 LYL1 TGFBR2 CHCHD10 ARF4 SLAMF7 TMSB10 S100A13 LPCAT4 AC104699.1 LGALS1 UCP2 MMRN2 ERG CDK2AP2 GYPC IL32 IVNS1ABP SH3BP5 TMEM59 RPS9 HLA-DMA CTGF STXBP6 ALG5 NDUFA4 SELT F2RL3 BST2 C16orf74 COX5B LAT2 ENPP2 CAV2 SRPRB DUSP5 IFITM3 WWTR1 SMAD1 CIRBP RPS13 BFSP2 EXOC3L2 CLIC2 FTH1 HNRNPDL GDI2 B2M IFIT1 TMED2 LRPAP1 HLA-DMB NOTCH4 TPD52L1 RGS2 PARK7 HHEX GABARAPL2 SOCS3 IGFBP7 MEI1 LGALS4 IFI27 GALNT15 RABAC1 RPL19 EPCAM S100A16 HLA-DQA1 CD74 RHEB MZB1 HES1 CYP1B1 SSR2 VIM SIT1 GMFG ICAM2 ARHGDIB RPL32 PLEKHF2 IL3RA HSPA1A DNAJB1 COX7C TNFRSF13B GAS6 IRF1 CYTIP COX6A1 RHOC IDO1 FBLN2 ZBP1 PTPRCAP OAZ1 COL4A2 HYAL2 HM13 SMARCB1 KRT18 MSN EIF1 AMPD1 COMMD3 LCP1 FSCN1 SELP MYL12A LSP1 HVCN1 HHEX LIFR RHOC PSENEN C15orf48 MYCT1 S100A16 GSN RPS25 KRT8 ACE TCF4 IFI27 ARL6IP4 ITM2B TSPAN7 MPZL2 REEP5 EMC4 MBD4 EPAS1 YBX3 TMEM208 ARPC3 BIK FAM110D EGR1 SDC1 ATP5O TXN C9orf3 ARL2 GLA MT-ND4 CCND3 CALCRL MTUS1 TUBA1A GMFG DEF8 HLA-DRB1 B2M EEF1D SRPRB RASGRP2 SOX18 SNHG7 KDELR2 ATP5B MARCKSL1 FABP5 FAM110D B4GALT3 NDUFA1 NEIL1 GALNT18 CALCRL PDE4B RPL37A SUGCT ITM2A ELTD1 RGCC RAC1 RP11-64H13.1 A2M PIR LGALS1 EIF3F RFTN1 IFITM1 JUNB RGS1 DNAJB11 ITM2C IGFBP6 IL3RA LGALS3 ATP5J MT2A NOSTRIN RNASE1 PDK1 MT-ATP6 TNFAIP8 JAM2 IL33 TMEM176B RPS20 ZCCHC7 RNASE1 VGLL4 SH3BGRL3 MGAT1 LINC00926 MYL12B IFIT3 IFITM3 CRELD2 AIM2 SLCO2A1 EFEMP1 KIAA0125 UBL5 STK17A CALM1 AC116035.1 MYL6 MT-CYB CISD3 NES KLF4 SRGN SELM CYB561A3 KANK3 TESC RP11-92E3.2 VAMP2 SLBP ARHGAP18 EPCAM TRIB1 OSTC TMEM156 RND1 STOM CITED2 ICAM2 BACH2 FTH1 CD55 ID2 EMP3 LMNA CLIC2 RND1 EVI2B NACA ATP1A1 LDB2 CDC42EP3 KRTCAP2 CALM2 GYPC MPZL2 TIMP1 BEX5 RPS3 RMI2 PEA15 HES1 CISD2 NDUFS8 PPP1CC MCAM TSPAN4 SEPW1 COX7A2 UBE2N DLL4 PLK2 ANXA1 PLP2 AGR2 MFNG ATP5G3 RPN1 CCR10 PARP1 C8orf4 TXNIP EIF1 TPD52 MME HLA-DPB1 HLA-DMA FOSB SELT HCLS1 BST2 BAG3 HAX1 ZNF706 PABPC1 PTPRB PDLIM4 IL32 PIM2 IGLL5 TSPAN4 MGP IFITM2 HINT1 RGS16 ACTN4 ID3 TMED4 UAP1 CD1C IPO11 PHGR1 SEMA4A SNRPD2 RGS19 DUSP6 TIE1 RAB30 S100A10 PAX5 TEK AGR2 SLC17A9 SLC35B1 ETHE1 GUK1 SEMA6A SLC38A5 REEP5 HLA-DQA2 ID3 HLA-B CAPZB TMEM66 DCK CDH5 TAGLN2 PTPRCAP ATRAID ITSN2 IMP3 KRT222 H3F3B SOD1 SH2B2 TBCD TMEM176A COPE RPS23 SUSD3 CABP1 SORBS2 WNT10A GUK1 SRSF3 GIMAP1 ST8SIA4 TMED9 TMED4 LYN JUP IFI16 CUTA RPS21 SYPL1 TNFRSF4 LGALS4 E2F5 DNAJC1 ARPC1B ARHGDIB GIMAP8 HSPA1A NDUFB2 CTSD PRX KRT8 SELT MT-ND5 IL16 GRB10 BAALC HES1 NUCB2 ZFAND6 PCDH12 FAM107A EZR PABPC1 PRPSAP2 NRP1 JUN DUSP1 RPL12 MAP3K7CL SRGN S100A13 RNU12 ATF4 S100A10 ERG ZFP36 PAIP2B DNAJB9 PXK NKX2-3 A2M SPINK2 B4GALT3 RP11-960L18.1 CLIC4 DTL SLC35B1 HNRNPA1 CCR7 TUBA1B EID1 SMARCB1 NEDD8 LSM10 SLC25A6 PKP4 SEPP1 CISD2 LYPLA1 LAYN CCL21 DNAJC1 KRTCAP2 DCAF12 TMEM255B HLA-DQB1 SEL1L ERGIC2 CTSH GIMAP4 LIMCH1 HSP90AA1 UQCRQ TMEM243 LIMCH1 GADD45B AC093818.1 CNBP TFEB THBD CD9 HLA-A LAMTOR4 AC079767.4 CD74 CXorf36 ICAM2 COX6C UBE2G1 HLA-DPA1 HAPLN3 TPI1 CD44 WIPF1 TSPAN12 VIM EMB LMAN1 KIAA0125 CDC42EP1 ADCY4 QPCT TMBIM4 HNRNPC COX7A1 WARS SPATS2 CST3 FXYD3 SCARF1 PLAT RHOH C4orf3 ID2 TXNIP ACVRL1 APOE EIF4A2 CBX3 SEMA3F MEOX1 MANEA FXYD5 SNAP23 RHOA CYB5A IRF4 NDUFB8 MOB1A LDHB INPP1 ANXA2 AUP1 DBNL SORBS2 LDB2 IFITM1 DDOST DOK3 TACC1 IL1R1 JSRP1 GSTK1 PLCG2 ITGA6 TMEM176B COMMD3 C19orf43 KRT19 KIFC3 ARL4A SRM PRDX2 IGJ LGALS4 CTHRC1 CXCL14 SKP1 SQRDL TIE1 PRCP SMDT1 A1BG FCRL3 HLA-DRB5 IFIT2 MT-CO3 SAP18 RRAS2 PRDX1 TMEM173 RPS5 TMA7 CERS4 PELO FAM198B IL2RG UBE2D3 OSER1 TP53I11 FABP1 SRPR DHRS7 LMO2 SERPINI1 GPR146 ERGIC2 RPS15 TAGAP PPA1 MLEC PTMS LGALS3 FTL FAM101B MMP28 PLP2 PSMB6 BTK S100A6 SQSTM1 OSTC SDF2L1 ATP5I PPFIBP1 KRT18 CNPY2 CHID1 ANP32B RPL12 SERTAD1 S100A4 ATP5G3 PTPRC TMEM173 IFITM1 SRP14 RBM39 RCSD1 ANKRD65 LPAR6 PPIB LAMP2 TUBB4B PLXNA2 RASIP1 SIL1 ATP6V0E1 RPS4Y1 APLN ALDH1A1 GLRX ITM2B MLEC CD93 MX1 CD69 EVI2B GSTP1 ITGA1 PTPRB RPL28 EIF3H CCNI C10orf54 NKX2-3 SLC25A4 SEC11C HLA-A VAT1 PPP1R15A TMBIM6 UFM1 RP11-138I18.2 KLHDC8B NEAT1 S100A11 OS9 NPM1 PHGR1 IGJ TNFRSF4 C11orf31 SGPP1 TINAGL1 MEIS2 LGALS4 ANXA7 HSH2D CYBA GIMAP6 JTB CALM1 BLVRB ME3 SRGN RPL8 PSMB3 ORAI2 TNFSF10 CLDN7 THAP2 TPT1 TNFRSF17 SERPINE1 LAPTM4A COTL1 TAPBP ALOX5 RHOC PLA1A TIFA CHPF PTPN6 EPHX1 EPAS1 TXNIP ERGIC3 ACTG1 NDUFA12 SLC41A3 FCRLA DERL2 GPSM3 PTMA LAYN ENO1 HIGD2A MTMR14 CCND1 ASRGL1 CD151 15-Sep FAM65B GIMAP5 FOS BRSK1 ARPC2 TFF3 RPLP1 IFI6 ARPC1B NDUFB4 KLHL5 GPX1 CSF2RB A2M RPLP2 GRB2 RBP7 CSRP2 AC104024.1 ST13 GNG7 KRT8 C10orf128 LMTK3 JTB CCDC69 SEC14L1 DDX5 SSR1 ATP5D CR2 CHCHD10 GBP2 RNASET2 NUDT22 TMEM141 PRIG IFI44L COX5B GNL3 DDX39A PSMB5 TIMP3 SEC61A1 NDUFB11 SRGN ARHGEF15 EIF4A2 HSH2D NHP2L1 MEF2C SCARB1 EVA1C ATP5E ARF1 HLA-DRB5 PRKCH IDH2 DCN SEC61A1 LAMTOR4 MCF2L RAB13 CHID1 CHMP2A REL GPR116 NEDD9 MT-CO1 RPL14 KIAA0226L DYNLL1 DNAJB4 RP11-16E12.2 NPM1 PRDX5 HEG1 NR2F2 ERGIC3 ARMCX3 CCDC109B OSBPL1A CAPG TXNDC5 SRPR PPDPF ARL2 IPO11 Vitamin_metabolizing Endothelial_pericytes Enterocytes Tuft_cells Goblet_2 CD320 RGS5 RPL15 AZGP1 MUC2 RAMP2 HIGD1B RPS2 LRMP TFF1 CLDN5 CD320 RPL13 SH2D6 RPL13 PLVAP PLVAP RPS6 MARCKSL1 ZG16 SLC9A3R2 CLDN5 GUCA2A AVIL RPL10 GNG11 CRIP2 RPL10 BIK RPL15 IGFBP4 RAMP2 AQP8 SH2D7 RPS4X TXNIP CAV1 RPL32 HCK RPS2 ENPP2 ESAM RPS4X ANXA4 RPS18 CLEC14A GNG11 RPS19 PTGS1 RPS19 TMEM88 CD36 SLC26A3 ALOX5 RPL32 ESAM COX4I2 RPLP1 ANXA13 FCGBP CRIP2 NDUFA4L2 RPS18 KRT18 RPL19 SPARCL1 IGFBP4 PLAC8 IL17RB S100P HLA-E MGP CEACAM7 TPM1 CEACAM5 RAMP3 EGFL7 FXYD3 TRPM5 TSPAN1 CD59 TMEM88 KRT20 EIF1B RPL11 CAV1 SPARCL1 FABP1 BMX RPS9 VAMP5 RBP7 PRAP1 HPGDS RPS14 IFI27 IGFBP7 TSPAN1 POU2F3 FXYD3 JAM2 MYL9 CEACAM5 GNG13 RPL10A ECSCR SLC9A3R2 SDCBP2 HTR3E RPL35 SEPW1 TINAGL1 SRI PSTPIP2 LYPD8 EGFL7 NOTCH3 MS4A12 SPIB RPL12 BCAM CLEC14A PHGR1 PLCG2 RPS5 GIMAP7 TXNIP C19orf33 ELF3 MUC1 CD36 ENPP2 RPS8 MATK ENTPD8 NPDC1 JAM2 RPS9 KRT8 RPLP1 RBP7 SDPR RPL10A C11orf53 RPS8 GSN GIMAP7 CTD-2228K2.5 TFF3 RPL35A CYYR1 RAMP3 RPL35 EPCAM RPL26 SDPR TM4SF1 MISP RASSF6 CLDN4 EFNA1 ECSCR GUCA2B RGS13 RPS13 ICAM2 HLA-E RPS5 FYB TFF3 TM4SF1 CYYR1 TMEM54 CRYM REP15 EMCN IFITM3 RPS7 PRSS3 FAM3D IFITM3 SPARC SLC51B IGJ RPS27A MGP A2M RPL19 TREH RPS3 TSPAN7 GSN RPL11 SPINT2 GNB2L1 FKBP1A CALD1 CDHR5 IL13RAl RPS7 IL3RA HSPA1A RPL5 NMU RPS16 IFITM1 CAV2 RPL35A SOX4 CLDN7 PODXL CCDC85B RPS13 DPYSL3 RPL6 IFITM2 VWF CLDN7 ASCL2 RPLP2 TGFBR2 VAMP5 RPL12 LGALS4 RPS15 STOM ZFP36 RPS23 HEPACAM2 RPS15A PPA1 HLA-C CEACAM1 LGALS1 MUC13 ENG HSPB1 CA2 HOTAIRM1 RPLP0 HES1 HLA-DRA ANPEP PLEKHB1 SDCBP2 CD34 EGR1 LYPD8 CLDN4 RPL8 VWF TM4SF18 KRT8 PPAP2C ELF3 HLA-C IFI27 LINC01133 PPDPF GDPD3 RBP5 CSRP2 RPS3 PTPN18 NACA CAV2 JUNB RPS12 OGDHL RPS12 SLC14A1 NOSTRIN RPLP0 MDK RPL23A PRSS23 FOS RPL26 FXYD3 RPL5 PLAT CDH5 GNB2L1 OCIAD2 CLDN3 CDC37 RNASE1 SFN RP11-39B14.5 PHGR1 A2M GADD45B RPS15A CLDN3 RPS23 CCDC85B IFITM2 RPL14 ESPL1 C19orf33 TNFSF10 FRZB RPS14 FABP1 GUCA2B EPAS1 IER2 PRSS3 ALOX5AP PLAC8 RNASE1 ENG LGALS3 ANXA3 RPL4 OAZ2 CTGF RPL6 CD74 BCAS1 SRP14 JUN RPL4 FURIN RPS6 CTGF ICAM2 RPS16 PPP1R1B RPL13A HLA-DRB1 BGN RPS15 MT-CO3 TBX10 GIMAP4 TPPP3 RPL23A ANKS4B TUBB2A HLA-DRA FOSB PTMA HSPB1 TM4SF5 ELTD1 RBP5 PKIB NCMAP SMIM6 ITM2B HLA-DPB1 RPS27A DEFB1 VSIG2 FAM107A HES1 AMN ZFP36 SERPINA1 AC011526.1 HLA-DRB1 RPL27A CC2D1A IFI27 APP HLA-DRB5 GPA33 COX5A LGALS9B MPZL2 MGLL GCNT3 MT-CO1 KRT20 IGFBP7 SLC14A1 PRDX6 EHF ZG16B TMEM204 SEPW1 AGPAT2 CALM2 MT-CO1 GPR146 EPAS1 AOC1 SOX9 PTMA CD74 FKBP1A SULT1A2 IFT172 SERINC2 FLT1 ITM2B MEP1A 7SK RPL14 C16orf80 SNCG RPL8 ITM2C TRIM31 ACVRL1 C8orf4 RPL31 CASP6 RPL24 FAM167B SOCS3 SMIM22 EMP3 AMN MMRN2 LDB2 TMIGD1 COX6C TPSG1 MGLL ELTD1 KRT19 ATP1A1 FFAR4 HLA-DPB1 PLAT CA4 PHGR1 KLK1 NOSTRIN EMCN CLDN3 CCDC115 TMEM54 GIMAP1 ID3 SERINC2 GFI1B RPL27A BST2 GIMAP4 RPL13A HSPA1A RPS20 HYAL2 PRSS23 PIGR S100A11 CDHR5 TIMP3 BST2 NEAT1 KIAA1324 CLTB TM4SF18 CD59 RPL29 EPS8L3 RPL29 HHEX FAM167B FTH1 NREP CREB3L1 GIMAP5 TSC22D1 TST HLA-DPB1 RPL3 RPLP1 HSPA1B CLCA4 HLA-DRA EPCAM SLCO2A1 RGS16 RPL7A HLA-DRB1 FOXA3 SNCG PDGFRB PPP1R14D MYO1B RPL31 FAM213A ADIRF MUC12 B2M CAPN8 HLA-DPA1 GJA4 MUC13 GADD45B GPA33 HEY1 TGFBR2 TMEM171 KLK11 CFDP1 SOX17 KLF2 HIST1H1C CLRN3 TMSB10 PTRF MFGE8 CLDN4 ATP2A3 RPS25 EMP2 APP C2orf88 NDUFB4 RPS24 RPL12 PODXL TRIM31 COX7A2 AQP8 NKX2-3 TIMP3 MYO15B S100A14 KRT18 SYNPO HLA-A ETHE1 EIF5 RPL30 SOCS3 BCAM RPL18 PRDX2 FAM177B NRN1 SLC2A3 RPS25 CYB5A RPL18 RPLP0 DNAJA1 S100A6 C15orf48 LGALS4 IFIT3 MCAM RETSAT CLDN7 RPL7A CDH5 SERPING1 RPS20 CHPT1 SPATS2L HLA-A CD74 CES2 CKB KRT8 IER2 SYNPO CA1 COX7C PRR15L TSC22D1 ISYNA1 RPL24 SLC25A6 PRSS3 RND1 COX7A1 RPL3 MAP7 DHRS9 KANK3 LHFP RPL28 VSNL1 PIGR THBD SRGN C11orf86 MT-ND4 NEAT1 NQO1 THBD SPINT2 BUB3 PLA2G10 C8orf4 EFNA1 RPL30 KRT19 EEF1D LDB2 MMRN2 RPLP2 CCDC28B RPL27 ARHGAP29 HLA-DPA1 CYSTM1 SRI SCNN1A C10orf10 FAM107A SLC26A2 SMIM22 FABP1 EHD4 IRF1 MT-CO1 FBP1 RPL28 HSPB1 CLIC2 RPSA H1F0 SMIM22 HLA-DRB5 PTRF COL17A1 ALDH2 FAM101A GABARAPL2 CYGB S100A10 PAFAH1B3 FTL NOTCH4 RPLP0 LINC00035 MAOB FAU GPR116 PPA1 MYH14 HLA-DRB5 HIST1H1C HEG1 MYCT1 EPCAM HLA-DMA PARM1 CLIC2 H3F3B RPS24 ACTG1 CEACAM6 SRGN B2M C15orf48 MIEN1 CEACAM7 FABP5 SPINT2 NACA MT-CYB GSN NFIB GPX3 HSD17B2 HOXB6 ARL14 AIF1L TSPAN7 SLC17A4 TIMP1 MISP ADAM15 COL18A1 TMSB10 GPX2 CA2 NOV FLT1 RPL36 ZFHX3 GUCA2A C9orf3 SOD3 EEF1D CD9 MLPH S100A16 EIF1 SLC44A4 MALAT1 CEACAM1 SH3BP5 COL1A2 CDKN2B-S1 RPL37A SPINT2 HLA-B PPAP2B LGALS4 NCK2 YBX1 B2M TCF4 IFI27 TAS1R3 RPL36 PIK3R3 SERTAD1 PPDPF PIK3CG SCGB2A1 PLLP STOM BTNL3 RBM38 C15orf48 C10orf54 C16orf80 NPM1 LDHA NAAA SPARC HLA-DMA BTNL8 COX5B MT-ND2 CFI APOLD1 ELF3 ESPN RPSA GAS6 NRN1 HN1 ESYT2 CLDN8 PPAP2A HES4 POLD4 PSMD9 ASS1 LY6E SOX17 ST14 ANXA2 S100A6 SERTAD1 LGALS1 SLC6A8 MT-ND1 POLD4 TIE1 ZFP36L1 CLTB TXN MXD1 MYCT1 REM1 LAMB3 STMN1 PFDN5 TMEM109 ID1 SLC51A DEGS2 SLC25A6 CD93 NPDC1 CLDN23 PMM1 MYO15B RPS2 AC011526.1 CDHR2 HOXA11-AS MLLT3 GIMAP6 CFI TMEM45B IP6K2 TP53INP2 ID1 CYB5R3 TMEM37 TMEM176B RPL18A TAGLN2 EFHD1 CHP2 ZNHIT3 UBA52 ZFP36 OAZ2 GPRC5A ATP5B MT-CO2 S100A13 CD34 HPGD IFITM2 ST3GAL4 CYBA NES CKB RPL36 ITM2C TACC1 SRP14 FCGBP HMX2 ATP5G2 LAP3 HHEX AK1 TSC22D3 LMO7 CFLAR TMEM204 ASS1 ACADSB RPL34 HSPA1A C1QTNF1 PRR15 S100A4 AGR2 LMCD1 GABARAPL2 ITM2C RHEB AC009133.21 TINAGL1 COL3A1 TMPRSS2 SPINT1 SYTL2 DLL4 MYH9 YBX1 IMP4 RAB27A TNFRSF4 DNAJB1 S100A11 LSMD1 RPL37 PTP4A3 PHGR1 PRR13 ATPIF1 CKB KDR LGALS4 KRT18 ADH5 VILL SPTBN1 ITGA7 DHRS11 H2AFJ CA4 HLX HEY1 HNRNPA1 IGFBP2 LINC01133 ROBO4 FAM222B GNA11 RAB4A RP11-94O2.2 PTPRB HSPG2 NDRG1 SPATS2L S100A14 IFI6 GPR116 CCL15 AFAP1L2 MEP1A FAM110D TACC1 RPL27 WFDC2 CYBA ATOH8 BBX SPINT1 DNAJB1 MT-CO3 APLNR SH3BP5 DEFB1 SKAP2 PKIB LPAR6 C10orf10 CFDP1 HLA-DQB1 KCNK1 PRMT1 EHD2 DHRS9 ANXA5 MAST2 PALMD TNS1 PFDN5 RPL31 EIF4A1 COL15A1 FAM213A PTPRH PBXIP1 CLDN23 SEMA3G LCN6 FLNB COL27A1 HPGD NDUFA12 PPP1R14A ACAA2 MT-ND5 SMIM5 RGS3 FAM110D PRSS8 RAB25 MALAT1 TMEM255B RPLP1 RPS11 FRAT2 SPINT1 CHCHD10 SDCBP RPL37 AOC1 MT-ATP6 COX4I1 SOX7 C10orf99 GSTP1 PRSS8 CD151 GEM RHOC MT-CO2 CLCA4 ARL2 EMP2 RPL34 RTN4 MT-ND4 SLC25A6 LMO2 EIF4A1 TUBA1A RPS3A ID3 NEAT1 CDA RPS27L EEF2 SCARF1 TIE1 BLOC1S1 CCDC14 ST14 GALNT18 IGFBP6 HHLA2 FUT3 MUC12 LIFR COL4A1 AHCYL2 TP53I3 HIST1H2AC SWAP70 APLNR LDHB MCL1 RHOC RPL29 SEPP1 GDPD3 TSPO RP11-665N17.4 SEC14L1 PLK2 HRCT1 ZFP36L1 RPL37A RPS19 HYAL2 MT-CO2 CMTM8 MT-ND1 RPL10A RPS29 FAM3D PRDX5 TSPAN3 HLA-DMA RNASET2 ATP5G2 HES6 IGJ RRAS TAGLN2 FAM132A PTMA RPS11 LCN6 SLCO2A1 SLC9A3R1 NDUFB11 EIF1 WARS PRIG PKP3 CHN2 KRT19 EPHX1 KRT8 STAP2 TMEM63A HSP90AB1 DUSP6 RPS2 SLC22A18 RASSF7 BEST2 JUNB CXorf36 ESPN VIL1 RASEF PRKCDBP LRRC32 MT-CO3 MT-ATP6 AOC1 RPL18 RHOA VIM CERS6 SPDEF RALB GIMAP1 TJP3 ID3 LGALS9C SORBS2 LIFR PCK1 CDH17 NPM1 EIF1 HDAC7 CTSA TMSB10 PCK1 ALPL TSPAN4 BSG ARPC1B PABPC1 FOS C10orf54 ARL14 IFI6 NLN RPS5 CYBA TSPAN8 FAM200B SEPP1 TMEM173 IFIT3 ENTPD8 CDX2 VIPR1 CALM1 HEG1 CDH17 HOXB9 HNRNPA1 KLF2 GIMAP5 MT-ND5 COX6A1 GPRIN2 VWA1 NQO1 CDKN2B AP1M2 BTNL3 ADCY4 IL3RA PEX26 RNF186 QSOX1 NES PTPRB SLC25A6 RPS21 SMIM14 ETS2 KANK3 SLC25A5 SHC1 BTNL8 MGAT1 IFITM1 GGT6 CD14 ITLN1 SERPING1 NKX2-3 LSR DPP7 NEDD4L SNX3 TMEM176B NLN LYZ GPR153 COX7A1 GPRC5B RPL18A SEPP1 TDP2 ACTN4 TCF21 APOBEC3B PERP CYSTM1 CARHSP1 NDUFA12 PABPC1 RNF24 SH3BGRL3 ERG ARID5B EIF1 TBC1D2B CDHR2 RPS4X RAC1 IL32 MACROD1 PTPRF RAC1 TNFSF10 SULT1A1 MYO10 ISG20 CYB5R3 EPHX1 LMO7 RPS11 LSR LRRC32 PRKCDBP CGN IFITM3 FBXO32 IMP3 ITGA1 RPL37A EPHB3 OASL RNASET2 PLAU S100A14 ASMTL RPL23 BTNL9 FAM162B LLGL2 YPEL5 CYP3A5 RPL13 DUSP1 IFITM3 H2AFY2 SLC26A3 YBX3 ACTN4 MVP STK38 PRAP1 HPCAL1 APOL3 CLCN2 JUNB MT-ND5 RPS18 COL6A2 TPRN PPAP2A SLC44A4 ELK3 ROBO4 ACOX1 LACTB2 KCNK5 KLF4 UBC AKR1B10 TAGLN2 RASSF7 PVRL2 IGJ CA12 SMARCC1 H2AFJ RHOC WNT6 MT-ATP6 GAPDH CA1 SNHG7 TMEM255B MPST AC005355.2 STARD10 CTNNBIP1 COL15A1 TSPAN3 TMPRSS2 CDH1 RPL28 ADAMTS1 FAU C7orf55 STAP2 RASIP1 RPL10 PARK7 TSPAN13 STX19 HYAL1 PTMA C1orf106 SNX3 PLAUR

TABLE 1B Absorptive_TA_1 Secretory_TA Absorptive_TA_2 Cycling_A Goblet_1 TXN MT-ND1 FABP1 EPCAM TFF3 GPX2 B2M SELENBP1 LGALS4 KLK1 MGST1 TFF3 CA2 MGST1 ITLN1 EPCAM MT-ATP6 LGALS4 AGR2 FCGBP AGR2 PRDX5 C15orf48 C15orf48 AGR2 C15orf48 MUC2 S100A14 GPX2 CLCA1 PPP1R1B FCGBP PHGR1 KRT8 LRRC26 LGALS4 KLK1 KRT19 CLDN7 RETNLB HMGCS2 RPL36 ETHE1 CLDN3 MUC2 TSPAN8 AGR2 FXYD3 PIGR WFDC2 C10orf99 PIGR LGALS3 HLA-DPA1 SPINK1 UGT2B17 ITLN1 UQCRQ PHGR1 SPINK4 ATP5B GPX2 PIGR FXYD3 KRT18 CLDN7 ATP5G1 COX5B TXN REP15 S100A14 MT-ND4 MT-ND1 ARHGDIB ZG16 PHGR1 EPCAM MT-CO2 VIM SERPINA1 ELF3 LGALS4 COX4I1 ELF3 TPSG1 PIGR ZG16 C10orf99 HLA-DPB1 LGALS4 CDX1 MT1G MT-CO3 BST2 ST6GALNAC1 MT1G CLDN3 MT-ND4 TUBB4B FAM3D CLDN3 FABP1 MT-ATP6 CD74 KRT8 FABP1 PHGR1 MT1G KRT18 EPCAM FXYD3 KRT8 TST S100A14 STARD10 KRT8 CLCA1 ATP5G3 MT1G PHGR1 COX5A COX4I1 KRT8 ARPC1B SMIM22 ATP5G3 CLDN7 CA1 ATP5G1 FXYD3 KRT18 H3F3B TMEM54 HMGCS2 GMDS PRDX5 FXYD3 CHCHD10 KRTCAP3 HEPACAM2 CYC1 MT-ND2 ATP5G1 CD9 RNASE1 RPLP0 RPS14 SLC26A2 HLA-DRB1 KRT19 ATP5G1 MALAT1 TXN PPP1R1B MT-ND1 MT1E IGJ B2M CLDN4 CLDN3 SLC25A5 KRT18 CLDN7 TSPAN8 VSIG2 TIMP1 CLDN4 CES2 HLA-DRA C15orf48 LEFTY1 RPL37A COX7A2 SUCLG1 PIGR FAM3D RPS29 UQCR10 CDX1 CLDN7 UQCRH MT-CO2 COX6C NUPR1 ANXA13 KLF5 RPS18 COX6B1 FAM3D SPDEF CHCHD10 C15orf48 HMGCS2 CYC1 MT-CO3 CLDN4 MT-CO3 AKR1C3 FABP1 TMEM141 LGALS3 TSPAN8 CKB PRDX5 ANG SUCLG2 EIF1 EPCAM SMIM22 COX6C CD9 SPINK1 HSD11B2 LGALS1 ELF3 TSPO RPL35 AGR2 TMEM141 S100A14 KRT19 SMIM22 SMIM22 TMEM54 HMGCS2 SMIM22 SPINK4 MT-ND5 CKB BEST2 C19orf33 STARD10 AMN CST3 MB NXPE4 FAM3D MGST1 NDUFAB1 FABP1 B2M MT-CYB MT-CYB C10orf99 CREB3L1 SUCLG1 MT-ND3 COX8A ITM2C RPL36 ATP5A1 RPS21 C19orf33 TMSB4X GPX2 ATP5F1 CD74 TMEM141 ARPC2 CLDN4 GAPDH HLA-DPA1 COX6A1 HLA-DRB5 S100A6 COX4I1 HLA-C AKR7A3 SPINK1 RP11-234B24.2 COX5B WFDC2 MT1E PLP2 URAD RP11-519G16.5 ATP5I GOLM1 SPINT2 TCEA3 TMEM54 TMEM141 AKR1B10 HLA-DMA TSPAN8 ETHE1 ELF3 PRSS3 HLA-DMB MT1G UQCRC2 RETNLB CLDN3 MT1E TSPAN1 CA2 TIMP1 CISD3 COX5A TMEM61 TMEM141 HMGCS2 ATP5D ATP5B RAP1GAP HLA-E RPS3 MT-CO1 ECH1 C10orf99 CDX2 PPP1R1B MT-ND2 TUBA1A REG4 COX6C RPS15 CHP2 IGJ PRDX5 C1QBP TMEM54 H3F3B FXYD5 MT-ND4 RPSA KRT19 KRT18 SELENBP1 CCL15 KRTCAP3 MT1E NDUFA1 ETFB UQCRH OLFM4 ZFP36 VSIG2 HLA-DQB1 H3F3B UQCRFS1 RPL12 TIMP1 SRI NANS S100A10 KRTCAP3 COX7C KRT19 NPDC1 ATP5C1 COX5B FAM3D KLF5 MT-ATP6 H3F3B IGLL5 PDE4C IGLL5 MT-CYB GSN RPS9 EIF1 LGALS3 MT-CO2 MRPL12 MGST1 COX5A HADH IGJ CD74 C10orf99 LGALS1 CDX2 MT-ND2 CKMT1B RPL8 CD74 UQCRC1 IGFBP2 SLC25A6 ITM2B TSPAN1 SMAGP SPINT2 ARHGDIB RPLP2 CLDN4 TIMP1 EIF1 RPS2 CHCHD10 TSPAN8 ACTB C2orf82 MPC2 UBC SLC22A18AS LY6E COX5A SELENBP1 HLA-DRB1 CYC1 COA3 IFI27 RPS24 COX6B1 MT-ND3 COTL1 HES6 RPS18 ATP5D ATPIF1 IGFBP2 COX5B MAOA NDUFB11 UQCR11 ACADS TIMP1 RPL8 C19orf33 ELF3 PLA2G2A CDC42EP5 CKB S100A14 SDCBP2 STARD10 FOXA3 MPST HLA-DRA ATP5I CES2 S100A4 IGJ RPS5 IGJ TST PPDPF TRABD2A COX5A CDX1 LEFTY1 ZG16B ATP5O RPS12 TSPO CKMT1B MT-CO1 RPS6 RPL13 SRI ATP5G3 IL1R2 HINT1 ARHGDIB UQCRC1 CISD3 TMEM176B SPINK1 C2orf82 MGST3 ISG15 HSD11B2 HLA-DPA1 RPS8 S100A6 RARRES2 CD9 ECH1 RPS2 MRPL41 MPC2 BTG1 PHB TCEA3 TCEA3 HLA-E UQCR10 CES2 HLA-DPB1 NDUFB9 ECHS1 IFT172 AKR1C3 LEFTY1 COX7B CKMT1A COX6B1 CKMT1A ACTB ZFP36 UQCRQ TPM1 PLA2G2A LRRC26 ATP5J GGH ZFP36 RPL5 MUC5B ATP5B TSPO SERF2 UQCR10 NUPR1 SLC39A5 MPST TSTA3 IGFBP2 MT-ND5 KRTCAP3 ATP5F1 MGST1 COX7C CKB NXPE4 COX4I1 TSPAN13 COX6B1 UQCR10 GPT ATPIF1 C19orf33 LCN2 SELENBP1 MS4A12 CYCS MT-ND3 RPL7A RPL27A ANXA5 UQCRH ATP5G3 ZFP36 MT-CO1 ACADS ZFP36 FAM195A RPS8 UQCRQ SLPI MACROD1 ITM2B CMBL STRA13 PXMP2 COX5B RAB25 FAM84A RPL7A NDUFB2 STAP2 FTL PEBP1 RPL32 FAM162A RPLP0 CDX1 S100A4 RPS19 DBI RP11-519G16.5 STAP2 STARD10 CISD3 ARHGDIB COX6C DNAJA1 HLA-C TPSG1 PPP1R14D RGS10 TMEM54 IGFBP7 AMN GPX2 SLC44A4 FABP2 PPP1R14D URAD UQCRH NANS ATP5I HLA-DPB1 MT2A TMEM45B NDUFV1 CHCHD10 PDE4C RPLP1 CYSTM1 RPS18 ARPC1B RPS3A TSPO MYO1A B2M TSTD1 PCK1 COX6C CDHR5 NBL1 UBC GSTA1 RPL18 SLC44A4 ALDH2 PPP1R1B RPL26 DUSP1 DHRS11 GNAI2 DDX5 STAP2 HERPUD1 ADIRF C1QBP ACTB RPS3 RPS6 PPP1R1B S100A4 MLPH RPL10A TMSB10 CKMT1B MLEC ETHE1 SEPP1 RPSA MT1M SUCLG2 SH3BGRL3 ATP5I ARPC1B HLA-C MINOS1 KIAA1324 FAM162A DDX5 ITM2B S100A10 KRT20 UQCRC1 ATP5G3 PKIB OAZ1 HSPA1A TCEA3 UQCRH USMG5 PSAP STRA13 CHP2 NDUFA1 FAM195A ATP5I IFITM2 RPL31 ANXA5 FCGBP TIMM13 CKB ATP5D TIMM13 IFITM3 SEPP1 AC011523.2 RPL37A HLA-B MPC2 HSPD1 HLA-C SRI COX8A S100A10 RPL36 UGT2B17 HLA-DRB1 CDX1 MISP UQCRFS1 ENTPD8 SELK HLA-E STAP2 ATP5A1 COX4I1 TSPAN1 SEPP1 MGAT4B ANXA5 CST3 RPS23 CDC42EP5 SULT1A1 HLA-C RGCC SOCS3 SNX3 PYCARD S100A6 B2M RAB25 CYC1 ATP1A1 SFN RAB15 MT1X HLA-DRB5 DNAJA1 ATP5O CD74 COX6A1 MRPL12 ZG16 AP1M2 NDUFA1 NACA HLA-DMA ASL MT2A MT1E RPS29 IFITM2 NPM1 RAC2 ERI3 GMDS RPL28 MPST RGCC TST COA3 RPL38 MUC4 GSN ERN2 UBC RPS11 UBC STRA13 TNNC2 RPL36 DNAJA1 SLC26A3 ATP5J2 NEURL1 SPINT2 HLA-A SLC51B CA2 GSN ITM2C RPL37 URAD PEBP1 LGALS3 IFITM3 COX7C HLA-B TYMP CAMK2N1 RPL13A ETHE1 S100A4 PRDX2 SMAGP DNPH1 HLA-DQB1 HLA-E H3F3B IFITM3 ISG15 MZT2B CDH17 SQRDL TSPO SLC25A3 LITAF CKMT1A GJB1 CAPN9 UGT2A3 ISG15 ANPEP PBK MALAT1 SLC39A5 TRABD2A SLC25A5 RPL37A CDX2 RPL12 MZT2A ABCC3 UCP2 TMEM176A RPL29 TSC22D3 UQCRFS1 TPM4 IGLL5 FAM195A TSTD1 IGLL5 CHCHD10 SLC44A4 URAD ARPC2 DUSP1 TMEM98 TTC39A NDUFA10 ECI1 TRMT112 ADIRF COX7B SQRDL ETFB IFITM2 DDT OAZ1 HSPD1 MPC2 SHD AKR1B10 COX8A DDT IGFBP2 JUNB S100A16 JUNB IFITM2 PLA2G2A TSC22D3 PLEKHJ1 UQCRQ NUPR1 TST ATP5E LGALS3BP MARCKSL1 TPI1 GSTP1 TMSB10 ARPC3 SCNN1A NOX1 HIST1H4C TXNDC17 NOX1 LYPD8 ACADS SDCBP HLA-DRA EEF1B2 COX7A2 ATPIF1 DNPH1 SQRDL FAM162A CTD-2547H18.1 TSC22D3 RPL31 CIRBP RPS14 RASD1 TMSB10 SOCS3 SERINC2 GGCT CIRBP RPS27A S100A4 DDT RPS8 KRTCAP3 ANXA5 PRDX2 LDHB TCEA3 H1F0 PRSS3 RP11-357H14.17 NDUFB7 GMDS NXPE4 TFF3 COX7B CMBL RPS6 RPS24 GOLM1 HSPA1A IFI27 ETHE1 RPL37A RPS15A RARRES2 AOC1 LAMTOR4 PCBD1 HLA-B CLUH RAB25 MT-ND1 YPEL5 MACROD1 RPLP0 KLF5 RPL8 HLA-E PXMP2 MPST PCK1 SH3BGRL3 MUC1 TST SPINT2 SPINT2 HLA-B ITM2C COX7A2 TXN TCEB2 IMPDH2 ATP5G1 AP1M2 GSN NDUFA2 TUFM KCNMA1 TUBB UQCRC1 C2orf82 PXMP2 PRR15L IGLL5 CES2 HERPUD1 NDUFA10 RPL26 GJB1 RPL29 S100A16 LYZ HLA-DRB1 EIF1 ATPIF1 GSN PHB CYC1 ARPC1B ST6GALNAC1 HNRNPA1 VIL1 AGR3 CISD3 MGAT4B BCL2L15 NDUFA1 FFAR4 PKIB MLEC LAPTM4A ACTR3 AMN GPR160 REP15 UGT2B17 HINT1 RPS29 MRPS33 IFI27 STARD10 RAB25 SCGB2A1 DCTPP1 FBL EID1 IRF8 KLF5 AKR1B1 DNAJB1 NDUFB3 CHP2 DUSP1 CDH17 UQCR11 MRPL12 AKR1B1 DNAJC12 AKR7A3 RNASE1 ESRRA FCGRT MUC4 HSPA1A NDUFS5 MT2A RPS3 ATP5J2 RPS14 IMPA2 PNRC1 RPL26 RAB27A PLP2 DDT NDUFV1 RPL10A COX7C RGS10 MYL12A GJB1 HOXB7 IL32 MT-CYB RHOA MYO1D MAOA PSAP TKT RPL11 NAP1L1 AMN RP11-357H14.17 MDH2 RPL10A VIL1 TSPAN1 HLA-DRA ITM2B NDUFB7 DDX5 MT1M HSPA8 HLA-DRA RAB25 TMC4 MRPL12 MUC5B EEF1B2 SUCLG1 NDUFS7 ITM2B PLA2G10 DUSP1 FAM195A SOCS3 NPC2 MPC2 PSMB9 MUC4 MAOA NXPE4 DUSP2 AMN SFN KRT20 UQCRC2 TRABD2A AKR1B10 MT1X PLCD3 SDC1 DYRK4 FBL GCHFR SFN ACAT1 KLK15 NDUFAB1 MUC1 ROMO1 IFITM2 LXN DBI FKBP1A SSR2 RPS21 NDUFB4 MTCH2 RAB7A EEF1D HERPUDI C12orf57 RPL14 GMDS ITM2C RPL13 SLC12A2 RPL3 TMEM176B PADI2 TPM1 DCTPP1 RPL11 FOS NDUFB1 SH3YL1 TMSB10 RPS9 TRPM4 DPP7 HSD17B11 GADD45B Inflammato- Stem_cells Enteroendocrine Glial_cells ry_fibroblasts Fibroblast_pericytes B2M PCSK1N CRYAB VCAM1 RGS5 LEFTY1 CRYBA2 ALDH1A1 NNMT BGN TMSB4X SCGN GPM6B LUM CSRP2 ASCL2 CHGA PLP1 SOD2 NDUFA4L2 MT-ND4 PYY SPP1 CCL2 MYL9 LGALS4 SCG5 S100B TDO2 MFGE8 SMOC2 GCG FXYD1 COL3A1 TINAGL1 PRDX5 FEV PRNP C1S TSC22D1 RGMB MS4A8 PMP22 MFAP4 COX4I2 MT-CYB TTR CLU C1R FRZB FXYD3 CACNA1A TUBA1A MMP2 ADIRF GPX2 PRDX5 CD9 CTSK TPPP3 CDCA7 HLA-C MPZ PDPN HIGD1B MT-CO3 HOXB9 SPARC FBLN1 COL18A1 TSPAN8 FXYD3 NRXN1 DCN GPX3 PHGR1 STARD10 DKK3 CTSC SOD3 MT-ND2 RAB26 CYR61 RARRES2 IGFBP7 MT-ND1 B2M LGI4 GPX3 NET1 EPCAM LGALS4 MATN2 APOE CALD1 ELF3 PHGR1 TUBB2B SELM 4-Sep PIGR RAB3B ANXA2 CALD1 TPM2 HLA-C KRT18 PMEPA1 IFITM3 SERPINI1 MT-ATP6 MARCKSL1 PCSK2 TMEM176A NOTCH3 MT-ND3 MDK PEBP1 CYGB PGF KRT8 SLC29A4 GFRA3 DYNLT1 HES4 MT-CO1 KRT8 CAPS COL1A2 ACTA2 PPP1R1B EPCAM CALM2 ADAMDEC1 MGP EPHB3 ELF3 MYOT WARS ISYNA1 SMIM22 SST L1CAM TMEM176B PDGFRB KRT18 HLA-B S100A1 COL6A2 SPARC HSPB1 TMSB4X COMT CFD FAM162B CLDN7 ARX CD59 GGT5 HSPB1 CLDN4 VIM PLEKHB1 NDN H2AFJ RPS18 CLDN3 TIMP3 FOXF1 BCAM C15orf48 HLA-DPA1 CDH19 NINJ1 PLXDC1 HMGCS2 C15orf48 SMIM5 PLAU CD36 HLA-B FABP1 TSPAN11 LAP3 CAV1 RPS24 RPL37A NTM EMILIN1 DSTN RPS21 MLXIPL C8orf4 IGFBP7 PRSS23 CLDN3 COX6C CNN3 STMN2 REM1 RPL36 C19orf77 MAL CXCL14 LHFP SPINK1 HLA-DRA FIBIN EPSTI1 COL4A2 RPL37 NEUROD1 FBLN2 HAPLN3 RGS16 MT-CO2 CPE CCL2 CD63 LURAP1L RPS6 SMIM22 CBR1 GBP1 TPM1 SLC12A2 TSPAN1 FGFBP2 SPARC TAGLN RPL37A HLA-DRB1 ARHGAP15 COL1A1 EGR1 S100A14 TFF3 LGALS1 PKIG IFITM3 RPL31 IGJ JUN LGALS1 HLA-C RPL12 HLA-DPB1 PRKCDBP SERPING1 EHD2 MT1G CLDN4 SNCA CFH MEST BST2 ITM2B RPS6 DMKN PKIG ACTB SEPP1 IGFBP7 SERPINF1 LGALS1 MARCKSL1 IFITM3 NDRG2 PAQR5 STOM PDZK1IP1 RTN1 COL9A3 THY1 A2M MGST1 SPINK1 ST6GALNAC2 SOD3 STEAP4 RNF186 LDHA TTR COL6A1 PTGIR GNB2L1 VWA5B2 TMEM176B CNOT4 RPLP2 RPS3 CD74 RPS2 LINC01082 PTK2 RPLP0 RPL36 FOS TNFRSF1A RBPMS ETS2 SOX4 AP1S2 PMP22 EPS8 HLA-A SCT WISP2 GSTT1 PPP1R14A CD63 BEX2 HES1 SGCE SRGN CST3 ISL1 VIM TPM2 COL3A1 ARHGDIB ANXA5 RGS16 A2M GEM FAM3D GSN FEZ1 TFPI CRIP2 MT-ND5 RPS29 SORBS2 CLEC11A ZFP36L1 CKB S100A14 FCGR2B FTH1 ARID5A RPS4X HOXB8 IFITM3 MFGE8 ARVCF GSN CHGB RP4-792G4.2 SPON2 EPHX1 C10orf99 GUCY2C RHOB GBP4 HLA-A FABP1 FXYD5 TMEM176A C2 ADAMTS1 ALDH1B1 CLDN7 ART3 SFTA1P PRKCDBP MT1E HLA-DMA EGR1 LAPTM4A MAP3K7CL TRABD2A HLA-DRB5 RPL8 TIMP1 NDUFAF4 KLK1 KRT19 TUBB2A CDH11 C1R SELENBP1 PRDX2 PDLIM4 LY6E CALM2 STARD10 SPINT2 IL11RA PLAT C8orf4 AGR2 EIF1 RPS19 CEBPB SDC2 RPL26 ETV1 ANXA5 APOL1 TCF21 SPINT2 HLA-E SOCS3 PROCR ESAM ARPC1B QPCT RPS18 TMEM205 HEYL KRT19 KIF12 PHLDA3 GADD45G KNOP1 RPS5 DDC NRN1 EVA1A EFHD1 RPS2 LITAF TSPAN15 ICAM1 SERPING1 RPL13 TMEM141 MIA FHL2 RCAN2 TFF3 TMEM61 COL18A1 KLF6 C1QTNF1 S100A11 MT-ND3 RPLP1 LGALS3BP RBPMS2 MYL6 COX5A SPARCL1 RCN1 SERPINH1 AQP1 IGLL5 TPT1 BST2 NDRG2 FERMT1 LY6E C1orf198 CCL8 FXYD6 MT-ND4L MPC2 SCCPDH GALNT11 COL6A1 RABAC1 IFITM2 S100A10 IGFBP3 GPRC5C HLA-DPA1 UCP2 S100A4 ECM1 MAP1LC3A RPL29 NDUFB11 RPL11 CYR61 RERG LY6E COX6B1 RASSF4 F3 GUCY1B3 HLA-E HEPACAM2 TNFAIP6 HSD11B1 ASPN SLC25A6 HLA-A SGCE CEBPD EPAS1 TIMP1 COX4I1 COL1A2 IGFBP6 CTSF RPL8 CXXC4 NNMT EFEMP2 UBA2 CD74 KIAA1324 CADM4 SEPP1 GUCY1A3 RPL35A TPH1 TAX1BP3 PRR24 RPS14 RPL10A VAMP5 RPL19 COL18A1 LRRC32 KRTCAP3 ATP5G1 RPS3 NAB2 MSC UBB RPS9 TFAP2A SCARA5 NR2F2 RPS12 MT-ND4 RCAN1 TNFAIP6 LGALS3BP KLF5 SLC25A6 IER2 TNIP2 ANGPT2 NOS2 MT-ND1 MYL9 TCF21 CD151 RPL5 ERI3 RPS14 PRR16 SORBS3 OLFM4 ZFP36 GPNMB IFI35 MCAM SOX4 S100A11 TUBA1B PTGIR COL1A2 RPL32 RPS14 GPX3 BRCC3 GNG11 RPS23 NPC2 FAM210B EID1 PTMS SEPP1 PCBD1 ID3 POSTN MYH11 GUK1 RPS21 CADM2 PSMA2 RNASET2 COX5A CKB GATM APOC1 RPLP1 RPS8 ATP5G2 HSPB2 CXCL1 THY1 MLXIP GPBAR1 RHOC S100A13 TGFBI CEACAM5 SELENBP1 RPLP2 CD302 COL6A2 RPS19 NDUFA3 RPL18 RBP1 ASAH1 QTRT1 SMIM6 NGFR EMP3 PLOD2 IFITM3 RPS11 HSPA2 BSG RARRES2 STXBP6 KLK1 ASPA SPG20 EFEMP1 RPL14 BAIAP3 FST TNFRSF11B SOCS3 CDX1 RPS2 MARCKS UBE2L6 RPS18 RPL30 RPS18 KCNMB4 IL7 RPS19 RPS9 RPL12 SBSPON PSME2 LBH RHOC MYL12A PSAP SCT SELM RPL7A TM4SF5 OLFML2A IL11 NEXN CDX2 CADPS RPL10 SRGN CDS2 HLA-DRB1 C21orf58 SEPP1 IGJ GADD45B IFI27 DNAJC12 C1S ARID5B COX7A1 RPS14 CTSC RPL13A EDEM2 FKBP7 IFITM2 PPT1 CXXC5 PSMA4 HLA-B TXN RARRES1 S100A6 TAP2 CD248 RPL34 RPS3 EMP2 IFI6 PTRF ISG15 DNAJA1 RPL13 FBLIM1 F2R HLA-DPB1 SNX3 MXRA8 COL5A2 MRVI1 IGJ NGFRAP1 SERPING1 FOSB NFASC PFN1 ISG15 RPS4X ATP5E PPIL4 AP003774.1 CDX1 RPL31 PCOLCE STK16 GPR160 RPL38 RPL28 COL14A1 SMDT1 H3F3B C12orf75 SRGN ETHE1 NF2 CD9 TAX1BP3 FGL2 CDK2AP2 ATF3 CDHR1 RPS8 TBCB IFITM2 APOE HLA-DRB5 PPP1R1B ENTPD2 ANXA5 FLNA HLA-DMA LYZ SELM TRIM47 TUBA1A S100A4 HMGCS2 PHLDA1 TSPAN4 RRAD NUPR1 PAM EID1 PDGFRA TRIB2 RPL18 PLA2G12A NGFRAP1 ISG15 OAZ2 RPL27A ACTB ANGPTL7 CD276 RPL19 RPS15 SPINK4 RPS8 ADM HRC HLA-DRA IFITM1 RPL26 APH1A HCFC1R1 RPS15A COX8A JUNB IL34 HEY2 ANXA5 IGFBP2 SLITRK6 FILIP1L C11orf96 RPL38 TSTD1 RPS12 MAD2L2 LAPTM4A TMEM54 LYPD8 RPL15 ADD3 RPL27A FXYD5 RPSA RPL12 TAGLN2 RPL11 RPL24 C4orf48 SLC22A17 PHGR1 ARHGEF17 RPS29 HLA-DQB1 RERG SQSTM1 CACNA1H PSMB9 GPX2 PCBP4 PLAC9 TGFB1I1 ARSE MLXIP CADM1 MESDC2 COTL1 RPSA LAP3 RPS23 NR2F1 PLEKHA4 RPL11 ATP5E ATF3 SERPINH1 RPS13 CTSC HSPA1A RPS27A NUBP2 GULP1 EEF1B2 AGR2 ITPR1 LAMA4 PARM1 ARPC2 TNNC1 LGALS3BP CYB5R1 OLFM2 CAPZB TPPP3 FSTL3 TSPAN9 RPS5 ZKSCAN1 SOCS3 RPS5 SEC63 RASL12 TYMP MT-ATP6 FAU DKK3 S100A10 KIAA1324 QTRT1 RPL32 F10 RPS6 LRIG1 HERPUD1 ZFP36L1 AGT ITGA7 IMPDH2 ETFB SOD1 COX5B DOCK7 GLTSCR2 MRPL41 SERTAD1 BBIP1 ANGPT1 RNF43 CD55 RPS16 TNIP1 CD74 RPS27A PEMT PCMT1 COTL1 CLMN ATP1A1 PRSS3 RARRES2 IFIT1 ENTPD3 PSME2 C10orf54 ITGB1BP1 IFITM1 RPL36 RPL23 CKMT1A RPLP0 PTGDS MAB21L2 RPS7 TCEA3 CTNNAL1 CD40 ILK DYNLL1 TYMP RPS20 ALDH1A3 COASY RPLP2 S100A4 HSPA1A ACP5 RPL28 LGR5 PSMB9 YWHAE NUPR1 MSRB3 OAZ1 RPL18 CST3 GSN CYGB SOCS3 RPS15 RPS9 OS9 PDE1A EIF3D MT1G SLC15A3 MRFAP1 FHL2 SUCLG1 RPL32 CLIC4 CLEC2B CCL2 HSPA1A PIGR DYNLL1 ARHGDIB ZNF580 URAD MT-CO3 RPS15A GNG11 CASC3 PTGDR CUTA RPSA NUMA1 SH3BGRL3 CHDH KIAA1456 MT2A PPAP2B HLA-F KCNN4 CTSD S100A16 LGALS4 TMEM98 PSMA7 RAC1 WDR86 SYPL1 RRAGA TAGLN2 QDPR DLX2 FBN1 LINC00152 C19orf33 C19orf45 GSN FABP1 LGI4 EPHB2 RPL13 LAMP1 TMEM119 MXRA8 ETHE1 WFDC2 ID4 MMP3 GPI PABPC1 HSPB1 POLR2F ATPIF1 10-Sep SELM RPL31 RXRG S100A3 MYLK ITM2B CD59 SECISBP2L C1RL CCDC146 IGLL5 OCIAD2 RPS7 AKR1B1 PTP4A3 MPST KIAA1377 TMOD2 HTRA3 NNT-AS1 UQCRH CENPV RPL6 NBL1 ARHGAP29 UBC EMC10 SH3BGRL3 SLC9A3R2 FILIP1 TDGF1 PLAUR DEPDC7 TYMP SCN4B PPAP2C DNAJB9 ERBB3 PUS3 FOS NQO1 RPL37 PON2 EZR RPS15 RARRES2 EPHB3 STARD13 PRKCDBP MOCS1 S100A6 GADD45B RPL23A ANG PPP1R15A HLA-DQB1 HIST1H4C SCD OLFML3 EPC1 TSC22D3 SERINC2 GRAMD3 CXCL6 FXYD5 CDKN1A CTSS AHNAK GPX8 VIM TGIF1 URAD CDC42EP1 CPQ SERTAD3 AP000344.3 RGS2 IFIT3 CCL13 RPL8 C10orf54 NDUFA11 RPL27A TNFRSF12A ID3 SH3BGRL3 ATP6AP2 RPL5 PGRMC1 HN1 WNK2 NUDT16L1 C1R PSMB9 EFEMP2 RPS2O SAT1 CMTM5 TPST1 EBF1 RHOA ANXA2 TNFRSF12A PAPPA TIMP1 MYL12A TIMM13 RPL29 FAM105A LPL COPE UQCR10 RPS29 COPA GNAI1 VAMP8 PRR15L ARHGAP12 EHD2 RSBN1L

TABLE 1C Myofibroblasts Villus_fibroblasts Crypt_fibroblasts_(hiFos) Crypt_fibroblasts_(loFos) T_cells ACTA2 NSG1 ADAMDEC1 CFD DCN TAGLN F3 CFD DCN LUM MYL9 FRZB DCN ADAMDEC1 CFD TPM2 CXCL14 C1S FBLN1 ADAMDEC1 PDLIM3 DMKN LUM LUM C1R ACTG2 VSTM2A FBLN1 MFAP4 C1S HHIP POSTN HAPLN1 C1R FBLN1 SOSTDC1 BMP4 CCL8 APOE TCF21 MYLK ENHO C1R C1S APOE FHL1 PLAT MFAP4 SOD3 COL3A1 HSD17B6 MMP2 APOE TCF21 CXCL12 MYL6 EDNRB CTSC COL1A2 MFAP4 TPM1 HSD17B2 CCL2 ABCA8 GPX3 MYH11 COL6A1 COL1A2 COL3A1 HAPLN1 DSTN COL6A2 TCF21 CTSC CFH CNN1 SDC2 COL3A1 CYGB SERPINF1 NDUFA4 AGT CYGB CXCL12 COL1A2 TGFB1I1 TMEM176B ABCA8 CXCL14 CCL2 NPNT IGFBP3 SOD3 CTSK PPAP2B DCN NBL1 STMN2 TMEM176B PLAC9 PDLIM7 CYGB CXCL14 GPX3 PTN PRKCDBP FENDRR PROCR RBP1 PTGDS WFDC1 RARRES2 GPX3 PROCR IGFBP7 CXCL14 FOXF1 CXCL12 COL6A2 PROCR COL3A1 MFGE8 A2M PLAC9 COL6A2 COL1A2 CAV1 RBP1 CCL8 CTSC SMTN ECM1 COL1A1 PTN CXCL14 FLNA TPM2 SERPINF1 IGFBP7 SOD3 HHIP-AS1 MFAP4 PTN LINC01082 CYGB C1S PDGFRA CCL13 CALD1 CCL13 SELM COL3A1 TMEM176B A2M CCL8 PPIC COL1A2 CTSK TMEM176A IFITM3 LUM GPX3 LINC01082 COL1A1 PMP22 PPP1R14A C1S PPAP2B SERPINF1 CCL11 ADAMDEC1 LGALS1 GSN IFITM3 RARRES2 COL1A1 CALD1 CFH CFH GSN TM4SF1 TMEM119 IGFBP7 ADH1B CD2 COL6A2 FAM150B CCL11 SERPING1 COL14A1 NBL1 WFDC1 CLEC11A CCL2 ADH1B NEXN APLP2 ADH1B CLEC11A SCARA5 LGALS1 COL1A1 GGT5 HAPLN1 A2M C1R BMP5 PLAC9 GGT5 COL1A1 ILK PDLIM1 SCARA5 RARRES2 FXYD1 KCNMB1 TMSB4X VCAM1 SCARA5 DKK3 SPARC SCPEP1 DKK3 CCL13 CALD1 CSRP1 PDGFD COL6A2 LGALS3BP CD3D MFAP4 MMP11 PMP22 GSN PPAP2A CALD1 MMP1 TMEM176A MMP2 ADAM28 IGFBP7 SPARC SEPP1 DKK3 TMEM176B LINC01082 TMEM176A MATN2 CCL11 CLEC11A HSPB1 IGFBP7 PPAP2A PMP22 CTSK APOE PROCR CYR61 PPAP2B EFEMP1 POSTN LGALS3BP CALD1 HAAO PCOLCE APOC1 PPP1R14A ADAM28 ADAM28 CD69 FBLN1 PKIG RARRES2 CD63 EMILIN1 TMEM176B IGFBP6 MMP2 PCOLCE STMN2 SPARCL1 TRPA1 BMP4 BMP4 MMP2 CAV1 TIMP1 SERPING1 COL6A1 GGT5 LMOD1 MYL9 VIM SEPP1 HAAO AOC3 MRPS6 SGCE SPON2 NDN CFD PCOLCE EFEMP1 SPARC SPON2 RBPMS SLITRK6 PCOLCE PPP1R14A RBP1 TCEAL4 C1R IFITM3 PPAP2A CD52 IFITM3 IFITM3 ECM1 FHL2 THY1 TUBB6 TCF21 LTBP4 LGALS1 BMP4 MMP2 SERPINF1 PTGDS PTGDS VCAN MXRA8 TGFBI LAPTM4A MFGE8 GNG11 CD151 REEP2 SPARC EMILIN1 SCT TCF21 SOX6 CD63 VIM PPP1R14A ACTN1 TSLP COL6A1 PRKCDBP ABCA8 PDIA5 CLEC11A PPP1R14A THY1 LAPTM4A PMP22 INSC SPON2 SELM TMEM176A EFEMP2 CTC-276P9.1 HAAO GNG11 LGALS1 LGALS3BP SRGN FOS LAPTM4A LTB CD9 RBP4 SNAI2 LTBP4 LINC01082 EMILIN1 LTBP4 NNMT TIMP1 PAMR1 TUBAlA PITX1 FHL2 STMN2 PLTP GSN LAPTM4A GNG11 EFEMP2 IGFBP6 MRGPRF EMILIN1 MEG3 SNAI2 NDUFA4L2 MFGE8 MAGED2 TM4SF1 ECM1 VIM COL6A1 GLP2R FABP4 SGCE SELM UBE2E3 LAMA4 EMILIN1 VCAM1 CIRBP C9orf3 A2M LGALS3BP IL34 FABP4 PTMS PROM1 EFEMP2 IGFBP6 S100A4 SERPINF1 RGS10 CXCL1 SPARCL1 QSOX1 JUNB LHFP LGALS1 NOVA1 RGCC RCN1 BAMBI PLAT FBLN5 FBLN5 FXYD1 RBPMS IGFBP6 NGFRAP1 PLAT CES1 ANXA5 SOCS3 PLTP MEG3 NUPR1 AKR1B1 TPM2 MATN2 SRGN RARRES2 BSG SMPDL3A FXYD1 TIMP1 SRGN PRR16 NDN EDIL3 GSTT1 FN1 MAP1B SELM TPM2 EMIDI SDC2 GADD45G FXYD1 SFTA1P SERPING1 FOXF1 TSPAN4 C2 TSPAN4 CD3E PCOLCE S100A13 PLTP MEG3 ANXA1 SERPING1 GLT8D2 VCAN EPHX1 LTBP4 SCPEP1 HSPB1 NGFRAP1 QSOX1 CCL5 AC131025.8 C11orf96 QSOX1 MYL9 SPARCL1 SGCE EFEMP2 SDC2 SRGN MXRA8 MIR145 FGF9 EPHX1 TM4SF1 IFI27L2 CRYAB EID1 GSTM3 EFEMP1 FN1 LTBP1 PTMS SPARCL1 PLAT GSTM3 CRIP2 COL5A1 TIMP1 OLFML3 MYL9 DUSP1 MXRA8 FHL1 GSTM3 PHGR1 CERCAM FKBP10 SRGN CCDC80 CD63 TPPP3 PTGDR2 COLEC11 DPT SEPP1 SH3BGRL CPE EDIL3 RAB13 TPM2 VIM SGCE IL34 ITIH5 GATA3 CKB TNC PRKCDBP NNMT TFPI NGFRAP1 TAGLN C11orf96 SDC2 LEPROT PTCH1 DCN ARHGDIB FSTL1 C16orf89 SOD3 TXNL1 FBLN5 LOXL1 SGCE COL4A2 EMID1 SFTA1P FABP4 LGALS3BP LRRC17 CRISPLD2 EID1 S100A13 LCK GNG11 SRPX2 FXYD6 COL14A1 DPT CYBA C1orf21 MYL9 NDN SNAI2 RBP1 NDN THY1 MXRA8 ZFP36L1 IER2 ISCU LINC01116 UBE2E3 IL32 CPQ CD9 TFPI FHL1 TSC22D3 MAP1LC3A ACP1 LOXL1 TAC3 LAMB1 BMP5 PALLD MXRA8 IFITM2 MATN2 OSR1 F2R IRF1 EID1 C6orf48 AKR7A2 BST2 PITX1 PITX1 SPARC NDN CPM MFGE8 C2 CNBP PKIG SELM UBE2E3 LRP1 NANS S100A13 PTN FGF7 NUPR1 FSTL1 HMG20B WNT5B SERPINH1 VKORC1 EEF1D RP11-332H18.4 SERPING1 OLFML3 APOC1 AEBP1 CFH RBP1 ARID5B FKBP10 SERPINH1 GAS6 FBLN1 PPIC FXYD6 NNMT FOSB NDUFA4L2 RAB13 LAMA4 WNT2B LPP PCDH18 CFL1 PPIC C11orf96 PALLD APOD JUNB DMKN PDPN TTLL7 KREMEN1 KCNS3 EMID1 GZMK IGFBP5 TUBAlA S100A13 NDUFA4L2 ELANE LAPTM4A ID1 CEBPD PLAU TRIM22 WLS ADM TSPAN4 FOXF1 CLEC14A EDNRB PRKCDBP APOC1 FN1 PITX1 FAM127A IFITM1 LAMA4 GLT8D2 SLC25A5 ARHGDIB CXCL12 C6orf48 COL5A1 CXCL1 CSRP2 TSHZ2 ZFP36L1 CTC-276P9.1 COL6A3 TIMP2 LRRN4CL GLT8D2 COLEC11 IDH2 MAMDC2 PTCHI NDUFA4L2 CFL1 COLEC11 P2RY14 LAMB1 EMID1 EHD2 COX5A S100A4 HHIP CCL7 RBPMS MXRA5 TRIP6 VIM SRPX COL18A1 EDIL3 SH3BGRL3 NNMT TIMP3 SCPEP1 EFEMP2 CBR1 CIRBP ANGPTL4 SMPDL3A PPIC MMP14 CAPZB SCPEP1 WFDC1 TDO2 SEPW1 CD63 DPT DUSP1 C4orf3 MFAP5 TGFB1I1 ADM COX5A VPS25 FENDRR IL32 GADD45B FOSB FNDC1 CALU PLK2 NUPR1 C6orf48 CYP7B1 TMEM176A TBX2 LRP1 SERPINE2 SPRY1 CTSK ANGPTL4 CYBA FAM127A PCDH7 C1QTNF2 PCSK6 RAB34 TMEM119 ZFP36L2 SNAI2 TSPAN2 PRNP GSTM5 DMKN COL4A1 WLS EGR1 CPQ ALDOA CD63 AEBP1 ZFP36 RAB34 COL6A1 COX7A1 SCUBE2 PROS1 AKR1B1 HTRA3 LOXL2 LANCL2 ITIH5 CD81 PRKCDBP CYB5R3 LOXL2 CD81 SLC9A3R2 CXCR4 FOS FIP1L1 CIRBP TNFAIP6 KRT8 IL32 RTN4 FOXF1 FILIP1L KLRB1 RPL28 ADH5 CCDC80 VCAN PHLDA1 CFL2 TM4SF1 NEGR1 TGFB1I1 FGF7 LTBP4 C7orf50 COX5A COL15A1 LAMA4 EHD2 IL1R1 NOVA1 ATRAID TAC3 ITM2C EMP3 FN1 TFPI COL18A1 STMN2 CYBA CPQ WNT2B SPINT2 BSG CAV2 ID3 SERPINH1 THNSL2 VCAN TMEM100 FKBP10 PRNP NEXN LAMB1 MAP1LC3A BST2 CTSF RNASE1 MAP1B IFI27 WFDC1 MDK FXYD6 VCL SEMA4D TDO2 ACTA2 LOXL1 P2RX1 PXDN DMKN CST3 CD81 WNT2B HAAO COL5A2 KLF6 TMEM66 PARVA NPY COL14A1 TGFBI CRIP2 S100A6 RGCC PGRMC1 TIMP3 TIMP3 ECM1 SGCB PHGR1 ABCA6 H3F3B TCEAL1 FHL1 SH3BGRL3 FGF7 IRF1 LAMA4 TPBG ANXA5 CYBRD1 ECM1 VKORC1 NUPR1 EHD2 MMP23B IFI27 NME4 TBX3 TAC3 EVA1A DDR2 TMEM98 RGS1 VASN PTMS SLC9A3R2 RPLP2 LEPROT SLC25A5 TNFRSF1A SGCA TIMP1 GNAI1 AEBP1 C7 CD74 CD74 MSC RBPMS RP11-14N7.2 COL15A1 PPP1CC PTX3 CCNI RGCC SFTA1P A2M ACTA2 CNBP CDH11 CDK2AP2 CTSS CD74 SPRY1 FGFR4 PTGER2 PTS LRP1 SEC11C BST2 FABP1 PPAP2A TMEM98 PLAU IGFBP5 TNFAIP3 TTC3 PLBD1 IFITM2 CXCL1 FGFR2 ADH5 CPQ 4-Sep CP FHL1 MCL1 VASN GSTM5 C16orf89 KRT18 FAM105A AMPD3 ABCA6 LINC01116 RND3 MAGED2 IGFBP5 FILIP1L CIRBP SCPEP1 NKX2-3 MXRA5 MT-ND2 SAMD11 MAPK10 RAB34 PHGR1 LEPROT SAT1 LY6E SGCA STMN2 FSTL1 SH3BGRL3 CLEC2B CCDC107 GULP1 MT-CO2 MIR497HG FTH1 SERPINH1 CCDC68 TUBA1A PHGR1 NUPR1 FILIP1L SPON2 HES1 HTRA3 CD5 MINOS1 CH25H CSF1 AEBP1 IL34 AEBP1 PLAU CDK2AP2 TMEM9 EMP3 NEO1 MRVI1 CDH11 S100A4 NUDT16L1 EID1 CD151 PFN1 SCT CCDC80 PDGFC CNTFR HTRA3 MXRA5 IL1R1 DCTN2 COL6A3 RND3 CNBP EVL CBR3 PDLIM4 HSPA1A IFITM1 RP11-14N7.2 RCAN2 CYTL1 JUN PDLIM3 CSF1 RERG COL4A5 MT-ND4 KCNS3 GNAO1 CLEC11A HMGB1 CST3 ISLR LRP1 FSTL1 ST5 HINT1 HSPA8 ITIH5 C2 GADD45B TNFAIP6 PFN1 MFGE8 FHL3 ID3 CHL1 BDH2 DUSP2 TGM2 CYR61 ADAMTS1 ELANE FHL2 MORF4L2 CTSF ACTA2 HINT1 TRAT1 TMEM47 CTSK SERPINE2 WARS FARP1 ISG20 ENPP6 C16orf89 COX7A1 MRPL23 ACTB LUM MYL12A PAMR1 TM4SF1 CD99 HOXA10 RCN1 LY6E LAMA2 EFEMP1 SERPINH1 IGJ CRYAB GZMA ZYX FILIP1L TMEM98 MYL12A PAM SAMD11 SEC62 ELANE SPRY1 RNASET2 SSPN GPC1 MAMDC2 IL6ST GPC6 RBBP7 ARPC1B CTC-276P9.1 ANGPTL1 IL7R CPED1 PDPN CD302 GAS6 IFITM2 RGS10 TUSC3 PCDH18 NENF FBN1 CREB3 RP11-332H18.4 FAM92A1 RUNX1T1 ACTA2 DDAH2 C12orf57 GRK5 CYBA RARRES3 SEPP1 NOVA1 WNT2B ANXA1 ADM MIR143HG WFS1 MDK NEGR1 FKBP10 NENF NGFRAP1 POSTN CYCS COL5A1 PITX1 CDH11 ISLR COL6A3 CCDC127 COL6A3 OLFML3 EPHA7 SLC25A5 GAPDH KANK2 ZFP36L1 ANGPTL1 PAM MGST1 NUDT4 PDE1A PHLDA1 IL32 VKORC1 ARHGEF25 ECHDC2 HSD11B1 CRIP2 HSD11B1 MMP23B BRK1 FTH1 TDO2 DUSP23 THYN1 HLA-A RGCC COL4A2 CHCHD10 RGS1 TCF4 IL6ST RGS1 SSBP3 ARPC1B SEC11C SMIM10 PCDH18 NGFRAP1 RCN3 COL4A6 TMEM150C P4HA2 ARHGAP24 SQRDL RCAN2 CTSF CYB5R3 EID1 APCDD1 SCARB2 ATP6AP2 TSTD1 ID4 RP11-532F6.3 MMP14 AKR1B1 EEF1D C11orf58 NDUFB9 SH3BGRL3 SVEP1 MT-CO2 CREG1 Macrophages Dendritic_cells Mast_cells Cycling_monocytes Tolerogenic_DCs FTL CST3 TPSAB1 FTL SNX3 C1QB CLEC10A VWA5A PSAP CPVL C1QC HLA-DPB1 LTC4S MS4A6A IDO1 PSAP HLA-DPA1 C1orf186 GPX1 CST3 C1QA HLA-DQB1 CPA3 AIF1 CLEC9A CTSB FCER1A SLC18A2 C1QA LGALS2 CD68 HLA-DQA1 HPGDS C1QC C1orf54 CTSD HLA-DRA MAOB C1QB HLA-DPB1 TYROBP HLA-DRB1 HDC CST3 DNASE1L3 SAT1 CD74 CLU TYROBP IRF8 LGMN AIF1 NFKBIZ IGSF6 HLA-DPA1 FCER1G LST1 RP11-354E11.2 CD68 CD74 MS4A7 IL1B SAMSN1 CTSB HLA-DQB1 MS4A6A LYZ GATA2 DNASE1L3 LSP1 AIF1 CPVL ANXA1 FCER1G COTL1 ACP5 AMICA1 GLUL MS4A7 HLA-DQA1 MS4A4A HLA-DMA FCER1A MS4A4A HLA-DRA DNASE1L3 TYROBP KRT1 NPC2 AIF1 GPX1 FCER1G CAPG LYZ HLA-DQB2 IGSF6 SPI1 CTSG IL1B HLA-DRB1 FUCA1 MS4A6A PPP1R15A VSIG4 SPI1 FCGRT HLA-DQB2 SLC45A3 LST1 LYZ SEPP1 HLA-DMB HPGD SDS HLA-DOB HLA-DMB CFP HS3ST1 CTSD HLA-DRB5 NPC2 HLA-DRB5 GMPR GRN HLA-DQA2 HLA-DPA1 IGSF6 KIT CPVL ACTB STAB1 LGALS2 RGS13 FGL2 LST1 HLA-DQA1 PLAUR CD9 SPI1 RGS10 HLA-DPB1 CD83 FCER1G HLA-DPB1 BATF3 RNASET2 IFI30 NFKBIA SAT1 CADM1 LST1 PLD4 BTK CD74 MPEG1 LYZ CD1C HSP90AB1 HLA-DRB1 ASB2 HLA-DRA MNDA CD44 HLA-DQA1 C1orf162 CD14 COTL1 MITF HLA-DPA1 PPT1 HLA-DMA GPX1 SERPINB1 RNASE6 FGL2 GPNMB HLA-DQA2 LMNA FAM26F S100A6 HLA-DRB1 ITGB2 ADRB2 PLAUR HLA-DMB PLA2G7 SGK1 VIM CTSZ BASP1 APOC1 GPR183 TYROBP HLA-DRA CD83 CD74 FGL2 SRGN HLA-DRB5 KIAA0226L SDS C1orf162 IL1RL1 RNASET2 HLA-DMA CTSS SRGN SDPR PLA2G7 SGK1 LAPTM5 FAM26F FAM46A SEPP1 TMSB4X CD163L1 LY86 BTG2 CD14 RGCC RNASE6 RNASE6 ALOX5 HLA-DQB1 PLEK VSIG4 RGS2 NSMCE1 STAB1 S100B HLA-DQB1 DNASE1L3 CTNNBL1 HLA-DMA SERPINF2 GRN CTSH MIR24-2 LAPTM5 ARPC2 ADORA3 CD1E LEO1 CLEC10A SMCO4 CTSZ FCGR2B SDCBP ACP5 ITGB2 S100A11 MS4A7 PTGS1 HLA-DMB HCK SPI1 LAPTM5 LAT2 AP2S1 CST7 PLD3 SAT1 ALOX5AP NCF4 UCP2 TREM2 CD1D FTH1 S100A11 WDFY4 FOLR2 C1QA DDX5 IGF1 CPNE3 CYBA CXCL16 AC020571.3 A2M TNNI2 CST3 ACTB DNAJA1 CCL3 GLIPR1 RNASE1 RNASET2 BACE2 ITGB2 DUSP2 ATP6V1F HCK CD69 SLC7A7 PTPRE CCL3 CACNA2D3 DUSP6 CD300A RNASET2 SLC40A1 CORO1A MLPH LGMN ARPC1B LIPA MPEG1 JUN SLC40A1 LY86 GLUL ARPC1B IL1RAPL1 TYMP SLAMF8 CSTB VSIG4 SIGLEC8 C1orf162 SLAMF7 CPVL BID RAB27B GLUL C20orf27 ASAH1 STX11 LAT RGS10 LIMD2 VAMP8 CTSS UBB VAMP8 FLT3 ATP6V0D2 FTL ACOT7 SRGN FAM49B RENBP SAMHD1 STMN1 P2RY6 PARVG CREG1 GLIPR1 FXYD5 C1orf54 CORO1A CLEC10A CSF2RA EGR2 MNDA BID FCGR2A CD68 ALDH1A1 AMICA1 GCSAM FAM26F LSP1 NCOA4 IFI30 RAB32 RGS10 INSIG1 GCSAML CTSH FAM26F TMSB4X IL8 CD33 FCGRT CD9 CTSL NR4A3 STX3 CSF1R LCP1 NCF4 ARPC3 SVOPL FCGR2A ARHGDIB AP2S1 DUSP2 ATP6V0A2 TGFBI CKS2 LY86 FAM110A LAPTM4A LGALS1 SUSD3 IGF1 CD33 HSP90AA1 MPEG1 PABPC1 HLA-DRB5 TMSB4X CD63 GPR183 FKBP1B FGL2 C1QC ANKRD28 SERPINF1 GSTP1 AKR1B1 CD86 LAPTM5 TBXAS1 PPDPF MALAT1 RGS10 EGR1 IL8 P2RY6 AMICA1 PHACTR1 ARL5B CTSS FCER1G APOE PPDPF CATSPER1 APOC1 NAP1L1 IFI30 AOAH HSPH1 RNF130 CD48 CD163 PYCARD KLRG1 HCK TYMP ITGB2 PTPRE CLIC1 ALOX5AP LAPTM5 HLA-DQB2 ARHGDIB TSC22D1 CD36 MT-ND2 S100A9 RNF130 S100A4 ADORA3 ID2 CD300A PLEK ATP6V1F SIRPA AMICA1 UCP2 TYMP CTD-3203P2.2 CYBA AIM2 CSF1R GRN SGK1 PLD3 CLNK OAZ1 NCF4 RENBP PDLIM1 LGALS3 GM2A TBXAS1 PLIN2 RGS1 IFI27 PLAUR C1QB PTPN6 GPNMB CSF2RA NPL ARRB2 ANXA2 CD4 VMO1 HCK IFI27 FAM212A RGS2 DUSP4 LILRB4 UCP2 FOSB TIMP1 ID3 C1orf54 ARL5B ASAH1 APOE SAT1 C5AR1 DUSP1 HSPA8 OAZ1 TLR10 LGALS1 CD48 ASRGL1 VIM TYROBP RNF130 RHOG LYL1 ATP6V0B MIR142 CD209 RGS1 EIF4G2 CORO1A GPR183 TTYH3 NR4A2 STXBP6 HLA-DQA2 TSPO PRDX1 NCF2 TNFSF10 CREG1 MNDA RAB42 HCLS1 GRAP2 HLA-DQB2 PFN1 IL1B ARPC2 NFKBID S100A9 LGALS1 FABP3 PILRA CSF2RB PPT1 GPX1 MPEG1 CD53 RAC2 LY86 HSPA1A CD36 P2RY13 NR4A1 TXN ACTG1 SLC7A7 CLEC4A HSPA1B EPCAM CCND1 NINJ1 PPT1 H3F3B LILRB4 CNN2 C3AR1 CHMP1B SMYD3 FUCA1 LTB CHMP1B GPSM3 MPP1 FXYD5 SAMHD1 CAPG ZNF385A FAR2 GNAI2 NAAA ADAP2 ATF3 LMO4 ADAP2 ITM2C OTOA LITAF SRSF5 CSF2RA HCLS1 CFD ZNF331 ARHGDIB LGALS4 TACSTD2 HSD17B14 PARVG EIF3D NINJ1 PSMB9 CD83 MIR142 EGR3 ATP5G1 XCR1 LILRB5 NAMPT CD82 FCGR1A PLCD1 P2RY6 P2RY6 MYADM EMP3 SERPINB9 CMKLR1 FAM49B TESPA1 KRT18 TMEM176B SERPINF1 FTH1 RASSF5 CAMK1 GMFG CTSC GAPT CALB2 PHGR1 COX7A2 BLVRA NPC2 BIRC3 CD163L1 CD99 TYMP ITGB2-AS1 HINT1 KRT8 PPM1J TBXAS1 HLA-DOA CD22 C3AR1 H2AFY RGS1 CYBA IL18 IFI27 PYCARD CXCL16 OAZ1 HSPD1 S100A4 RGS1 CD86 P1D1 STXBP2 RAB31 TMEM59 CD4 CCL3 MBOAT7 DAB2 SRGN A2M RILPL2 RGCC ANXA1 ZYX IL8 CXCR4 IER2 ATP6V1F CLEC7A C1orf162 CSF1R MSRA TUBB4B NABP1 NAGK ARL4C JUNB CD209 ZFP36L2 ATP6VOB PDLIM1 BHLHE40 TFF3 ABI3 HLA-DQA2 IGJ ARHGEF6 LSP1 MT-ND1 FTH1 NCF1 CST3 ARHGDIB CD37 CAMK1 G0S2 DUSP10 UCP2 FNBP1 GPR34 HSPA1A SCYL1 CXCL16 EVI2A SLAMF8 VAMP8 RGS10 HBEGF HAVCR2 S100A6 TNFSF13B PRDX6 ZNF331 ARPC3 IL18BP H2AFY ACTG1 FCGR2B CD63 CTSH OLR1 CHST2 CTSC HES1 ARHGDIB HCST CD37 RBI KIAA1598 PLTP MT-CYB DDX3X SRI VAC14 COTL1 TMEM59 ESYT1 YWHAH IGFBP7 ARL4C CXorf21 CRBN RENBP TAP1 FPR3 CNPY3 SYTL2 SGK1 LDLRAD4 SRGN EIF4A1 CTSD CD163 ELOVL5 HMOX1 THEMIS2 HNRNPM C5AR1 IL16 TNFSF13B C20orf27 P2RY14 LILRB2 RGS19 CYBB CD300A CD83 COTL1 DUSP10 LAIR1 S100A11 SLC2A6 CLEC4A PDLIM7 GLIPR1 YBX1 CKS2 TMSB4X TWF2 ITM2B LGALS1 ARHGAP18 LAIR1 CTSZ YWHAH IGFBP7 TIMP3 ASAH1 IFITM3 TGFBI ANXA1 TMEM154 EEF2 CXCR4 HLA-DOA PTPRC CMA1 PLD4 COX5B CCL4 AGPAT9 MALAT1 MAFB VIM DAB2 FCGR2A RGS1 RPL24 SELPLG EBI3 CTSZ DNAJB1 FCER1A CFL1 GATM PPIF FCGRT PLTP ATG3 ATOX1 DOK2 PFN1 TUBA1B C12orf5 FCGR3A MT-ND2 EXD3 RPS27A PNMA1 ARPC3 GNA15 LIF GMFG APOL3 TNFAIP8L2 KRT18 GBE1 AXL RAB31 ABI3 HERPUD1 CHORDC1 CLEC7A MT-CYB RHOG HBEGF GAPT PRDX5 MYCL RGS2 SCIMP HSPE1 CD83 IFNGR1 CCL18 LCP1 ITM2B HCST GYPC HN1 PTGS2 UBXN10 GNPDA1 GPSM3 RAC1 LIMD2 CNIH1 IGJ PLEKHO1 TMEM176B PMAIP1 SLC16A3 TUBB LSM6 KRT8 PABPC1 GNPTAB RPL31 MSL3 PYCARD KDM6B TSPO DUSP1 UQCR10 PILRA IL32 RPL28 RPL35A LGALS4 LGALS4 FPR3 MAML1 P2RY13 CXCR3 SLCO2B1 PFN1 TUBA1B CD9 CIITA SMS BSG UBE3A BLVRA BCL2A1 CORO1A GMFG NFE2L2 GLIPR1 ROGDI ZNF331 SLC31A2 SH3BGRL3 TNFSF13B TGFBI ARRB2 SNX10 ELF1 GATM MIR4435-1HG IFI27 SEPW1 PRKAR1A OSM CKLF SIGLEC7 ZFP36 ENPP3 CLDN7 IGJ GPR183 FOSB GALNT6 NCF1 BST2 DOK2 KYNU CCL2 CTSL DGAT2 CLEC4A RGS19 ACTR3 GM2A NDUFB9 CECR1 PHGR1 TMEM66 LRRC25 COX6C TMEM37 SDS NCF4 C15orf48 MT-ND5 RHOC AKIRIN2 BEX4 AKR1B1 KLF6 ANXA1 DSTN BLVRA RAB42 KRT18 PHGR1 VIM SERP2 GSN 1-Mar AP1B1 S100A4 TM6SF1 TREM2 EVI2B NCF1 RB1 ITM2A RPL34 CPPED1 GRB2 ARPC5 DHRS7 SLCO2B1 FERMT3 GAL3ST4 H3F3B IFI27 ADAMDEC1 ST8SIA4 ID1 PAK1 2-Sep TSPO PTPRC NINJ2 RAB32 CD84 TRPM2 GNAI2 SDSL CSF3R HSPA9 RPL18 ATP5J CD63 GSN FECH RPL5 GPR137B ABHD12 RAB31 PRDX5 H2AFZ HSPA1B GNPDA1 ID3 IFITM10 SDSL RNASE6 CD81 TNFAIP8L2 HSPA1A MT1E AKIRIN2 LRRC25 SOD2 DLC1 FABP1 LITAF YBX1 SLAMF8 HIF1A ENG TOMM34 GPSM3 CCL3L1 LYN TNFAIP8L2 PTPRCAP TFPT LILRB2 DDX3Y LIPA AP1S2 MKNK1 PRDX5 ZEB2 NCF2 BSG SLC15A3 ANXA5 RHOG ARL4C MT-ND4 BRI3 RABAC1 RBMX MGST1 MCL1 ADAMDEC1 S100A6 CDK5 GPSM3 ACTR3 IL2RA FCGRT DDX39A RAC1 CD40 IGJ COX6C TMSB10 CECR1 MT-ATP6 RBI CD52 EIF1 ARPC1B PPA1 MPP1 NGFRAP1 NEK6 PARVB KCNMB1 SLC7A8 PLEKHO1 CSF2 CYBB MAP4K1 TNFAIP2 RAB20 CSF1 VMO1 EPCAM SCIMP ITM2C CXCL14 SLC16A3 MYADM TFF3 CEBPD PIK3R6 DOK2 CAP1 NCKAP1L CD9 GPR65 TNFAIP2 SIGLEC10 FXYD3 CD151 RPS4Y1 ARRB2 CECR1 ARPC1B NUDT1 VAV1 ATPIF1 ACTN1 SIGLEC1 CCDC88A IL4R COX5B RAB7L1 TUBA1B MAT2A SELM ITGB7 FAM110A BSG PRMT10 EVL NAGK LINC00152 EEF2 GCA HNRNPA2B1 ATF3 INPP5D BST2 LINC00936 BCL2A1 IL1RN PHGR1 HCST COX5B RALB SUCLG1 GRN LGALS3 MCL1 CORO1A HSD17B14 AC093673.5 MNDA CARD9 RAB32 CD86 C12orf57 RAB20 REL WDR45B KRT19 PHACTR1 FCGR1A BCL2A1 LINC00863 TTYH3 CD86 PTAFR TUBA1B ABCB8 ANXA5 S100A4 CD53 FGR EIF2AK1 SOD2 DAPP1 HCLS1 ABI3 SAR1B BST2 RHOG LSP1 SOCS3 RHBDD2 CAPG CYB5R3 AGR2 IFNGR1 DHRS9 FOLR2 C10orf128 C12orf57 JUNB SEMA7A PRDX2 RHOF AOAH GHRL CCDC28A STX11 KRT8 STMN1 MT-ND5 TRAPPC2P1 SNCA ANXA6 GMFG NAGK IGFBP7 PTGS2 ITM2B IRF8 CIITA GPR35 CMKLR1 SCNM1 AXL CPPED1 PAK1 ATP5B PRDX5 MMP14 LGALS3BP PARVB RPL37A CAT C15orf48 KLF4 RARRES1 RASSF4 PTRHD1 TRPM2 WAS IL5RA S100A6 CD72

TABLE 1D Neutrophils Activated_CD4_cells_loFos Activated_CD4_cells_hiFos CD8_IELs CD8_LP_cells S100A9 RPLP1 IL32 CCL5 CCL5 SOD2 RPS3 ANXA1 CD7 IL32 IL1B IL32 KLF6 GZMA NKG7 PLAUR RPL10A S100A4 NKG7 CCL4 LST1 RPS25 CD69 HOPX GZMA AIF1 RPSA DNAJA1 IL32 DUSP2 SPI1 RPL32 HSPA8 CKLF CD8A G0S2 ANXA1 CD3D KLRC2 SH3BGRL3 LYZ RPLP2 RPLP1 CD160 CST7 SAT1 RPL19 LTB GZMB CD8B FPR1 RPS19 CCL5 PTPRCAP CD52 TYROBP TPT1 CD52 TMIGD2 GZMK FCER1G RPS15A ID2 HCST ZFP36L2 SERPINA1 RPLP0 SH3BGRL3 EVL HCST FTH1 RPL13 BTG1 CD52 HOPX FCGR1A RPL11 TNFAIP3 CD3D PFN1 S100A8 RPL28 TNFRSF25 GNLY TMSB4X IGSF6 RPS12 CALM1 CD3E BTG1 CFP RPL13A TSC22D3 SH3BGRL3 GZMB IL1RN RPL30 EIF1 RAC2 CD3D HLA-DRA RPS27A TMEM66 CTSW CD3E CTSS RPL4 CD2 PHGR1 GZMH TYMP RPS14 ZFP36L2 IGJ CKLF FAM26F RPS6 RPS3 TMSB4X MYL12A HLA-DQB1 RPL23A RPSA GAPDH CXCR4 FGL2 RPS2 CD3E CORO1A CFL1 CPVL CD52 TMSB4X ABI3 NR4A2 STX11 RPS18 RPS19 PRF1 B2M HLA-DRB1 RPL6 SRSF7 ACTB ARHGDIB CD14 LTB HSP90AA1 CD3G LYAR FTL RPL27A DUSP1 ARHGDIB ANXA1 HLA-DPB1 S100A4 MYL12A SIRPG RPL28 HLA-DQA1 RPL10A ARHGDIB LCK CTSW COTL1 RPL3 ACTB ACTG1 TMEM66 NCF2 RPS16 RPL28 RARRES3 C9orf142 HLA-DRB5 RPS5 CORO1A PFN1 PSMB9 LILRB2 IL7R RPLP2 CD247 RPLP2 APOBEC3A RPL31 PFN1 STK17A RPS3 EREG RPL14 ABRACL CAPG PTPRCAP C1orf162 UBA52 IL7R TBC1D10C LAG3 S100A11 RPS15 LEPROTL1 XCL2 CORO1A CDC42EP2 RPL18 RAC2 FABP1 HLA-B PLEK SH3BGRL3 B2M ARPC2 GZMM MS4A7 RPS20 CD47 CD96 IFNG LY86 RPS13 IFITM3 C9orf142 TUBA4A HLA-DPA1 RPL27 APRT LGALS4 ID2 IFI30 RPS8 HLA-DRA FTH1 S100A4 HLA-DMB EEF1B2 RPLP0 XCL1 RPS19 LGALS2 RPS23 IL2RG CD8A CD69 ITGB2 RPS4X TPT1 1-Sep CD7 C5AR1 RPL12 RPL10 CST3 ACTB SRGN ARHGDIB CD53 AC092580.4 HLA-A CYBA RPS3A DNAJB1 CFL1 CD2 TIMP1 RPL35A PTGER4 CST7 PSME1 CD74 RPL5 ID3 CLIC1 ALOX5AP CST3 RPL15 PPP2R5C PPP1CA RPL27A CD36 RPL37 CD40LG IL2RB HSPA8 TNFSF13B RPL8 HLA-DPB1 ALOX5AP LEPROTL1 MS4A6A TMEM66 CKLF TIGIT SRGN BID RPL34 RPS12 RPS19 HSPB1 GBP1 CD3D RPS27A IGLL5 SRRT GLRX RPL29 PHLDA1 PLEKHF1 RPS27A NFKBIA IGFBP7 RPL19 ACAP1 RPL30 MNDA PTGER4 FTL PTPN6 CXCR3 CXCL10 RPL35 DRAP1 P2RY11 CALM1 ACTB CD3E CD63 ID2 KLF6 FCN1 RPS7 DEDD2 MYL12A RPL13A IL8 TOMM7 GPSM3 FASLG CREM ARPC1B CXCR4 DDX5 CYTIP BIN1 HLA-DQA2 MYL12A 1-Sep KLRD1 RPL23A PILRA RPL18A UBE2D3 DRAP1 APRT LILRB1 BTG1 CFL1 CD8B RPS20 FGR RPL9 GRN CLIC3 HLA-C NINJ1 RPL7A PSMB9 IFITM3 CYBA CD86 TMSB4X TPM3 CXCR3 ABRACL LINC00877 CD63 CD48 PPP1R18 TC2N OAZ1 CORO1A RPL14 RPS4Y1 1-Sep TREM1 FAU PDCL3 ACTR3 CD99 ASGR1 CD2 SAMSN1 GRN EVL HLA-DMA TNFAIP3 PSME2 RGL4 ICAM3 TNFAIP2 RPL36 RPS6 TPI1 IFITM3 ARPC3 CCL5 SRGN COTL1 LCK CAMK1 EEF1D RPL32 TRAPPC1 C12orf75 S100A4 GPSM3 ALOX5AP KLRC1 ARPC2 CPPED1 LDHB RPS20 HSPA1A FYN RAB20 RPS9 ARHGDIA CIB1 XCL1 RIPK2 LEPROTL1 SOCS1 PSMB10 PRF1 CXCL9 PFN1 DDIT4 ITGA1 PSAP LAP3 KLF6 MIR24-2 LAT2 ATP5E ATP6V0B CALM1 HLA-B CD244 YPEL5 HCK CD69 HLA-DRB1 ITGAE DRAP1 GCA APRT PGK1 ENO1 MCL1 RP11-290F20.3 GLTSCR2 LAPTM4A BCAS4 CRTAM LILRB4 GPR183 FDX1 CDK2AP2 PPP1CA CD37 RPL26 RPL27A NFKBIA RPLP1 PRELID1 RPL36AL RPS4X PTMA RPS15A RNASET2 GIMAP7 CITED2 GIMAP7 GSTK1 GCH1 HSPB1 PSME1 RPLP2 TIMP1 CYBB ABRACL RAN NPC2 CLIC1 NCF4 PSAP MALAT1 ARPC1B ID3 IL23A HLA-DPB1 H3F3B VASP TMA7 RP11-701P16.5 RPL24 RPS15A LSP1 PTPRC SERPINB9 HLA-DRB1 FOSB HERPUD1 PPP2R5C MPEG1 PTPRCAP CXCR4 RGCC RGCC CCL3 KLRB1 BCAS2 PTPN22 RNF167 CFD IFITM3 ALG13 CISH MYL12B UBE2D1 HLA-DPA1 LCK MATK PSME2 THEMIS2 FTL RPL11 HSPA1B HMOX2 STXBP2 EVL CDC42SE2 SOCS3 RPL13 ARRB2 APOE RPL13 RPS3 CD59 GPX1 FXYD5 CACYBP RPL13A SAMSN1 TIFAB CD74 IDS PSME1 RARRES3 CORO1A HLA-DRA GALM PTPN7 TRAPPC1 DUSP2 DDX5 CD6 CD2 TAPBP TESC RPS4Y1 CCL20 ASB2 SH3KBP1 CD68 RGCC RPS2 OSTF1 APOBEC3G SPHK1 TC2N RPL31 DOK2 GLIPR2 KYNU HSPA1A UBE2D2 ITGB7 PSMB10 BCL2A1 CMPK1 IL4I1 MT-CO1 DHRS7 GLUL CD6 SLAMF1 CD59 RPL19 BLVRA IL2RG FOS TNFRSF18 TSC22D3 KDM6B SRGN MGAT4A RPLP1 MALAT1 NAMPT NPM1 TRMT112 FCER1G STK17A SLC31A2 TSC22D3 FAM96B LAG3 DENND2D NUP214 PDCL3 IL12RB1 HSPB1 RPL31 ABI3 ZFP36L2 SVIP ARL6IP5 ITM2A SELK CD59 CCR6 WAS CDK2AP2 PSAP CFL1 RPL36AL BUB3 MZT2A SAMSN1 SOCS1 PLP2 RGS1 RGS1 PPIF NACA CYCS CD69 SOCS1 ATF5 RPL38 TTC39C SLC16A3 GUK1 AMICA1 CKLF HLA-DPA1 HLA-DRA GRAP2 IGJ CD37 NOP58 RPS3A C19orf60 ITM2C SH2D2A ENO1 PTTG1 TNFAIP3 YBX1 GNB2L1 MYADM LDLRAD4 IL2RG ACSL1 IGJ RPS25 CD53 DDX5 RNASE6 BTF3 HNRNPA0 PSAP EEF1D ZFAND5 NPC2 JUN PTGER2 RPS12 GRN CXCL14 YPEL5 SH3BP1 ARPC1B WAS CCDC109B PPP1R15A CHMP4A PTGER4 TNFAIP8 LGALS1 SERP1 IDH2 ZNF331 JUN HSPA8 RPS14 RPS27A BUB3 ASGR2 CRIP1 EVL LSM2 RBM8A CXCL2 HSPA1B PSAP EEF1A1 CAP1 FCGR1B CCR6 FAU HCLS1 RPS18 LIMD2 RPS29 RPL13A MYL12B 7-Sep DOK2 PFDN5 PTPRCAP CRIP1 C19orf24 PFN1 TTC39C TAGAP PABPC1 HLA-DRB1 LILRA2 RPS21 DHRS7 LYAR FAM177A1 PYCARD C9orf142 H2AFZ FYN CRIP1 ISG15 RPL37A AMD1 BIN1 ABT1 KMO RPL17 CD74 RGS19 CXCL14 IL10 PABPC1 ODF2L DEF6 RPS25 CTSH EIF1 SND1 RPL18A SNRPB CD48 GSTK1 OSTF1 IFI27 RPS2 RTN1 ARL4A ERP29 LCP1 EIF1 IKZF1 YPEL5 PNP HENMT1 CTSB SH3BGRL3 CD7 ARL4A CXCR6 BAX C19orf38 HCST RPL30 RPL9 MFSD10 RIN3 LAPTM5 MRPL11 FCGRT RPL36AL PSME2 ITM2C AATF RPS10 RORA HCLS1 ID2 RPL4 CCL4 SRSF7 CD83 FYB MCL1 RPS27 HNRNPUL1 AP1S2 TUBA4A JUNB APOBEC3G COPE LCP1 1-Sep BAZ1A CD99 FTL ITGAX RPL22 EIF4A3 TPM3 C9orf78 PKM RORA CREM RPL17 PDCL3 CFL1 LAPTM4A SRSF2 GYPC TAGAP VAMP8 PLD3 RPS5 GSTK1 UBE2D3 IFNGR2 SNRPD2 MRPL34 IL2RG C14orf1 NPC2 METTL9 SNHG8 ATP5E PLP2 RILPL2 B2M C9orf142 GYG1 GPSM3 GPBAR1 CACYBP MTFP1 FOSB UBE2L3 CSF1R SAMSN1 RPS8 SASH3 GPR65 OSM HIGD2A PRR5 C19orf53 ATP6V0E1 CCRL2 ARPC1B ACTG1 7-Sep RAC2 CLEC10A 9-Sep CHCHD7 FXYD3 KLRD1 IL4I1 GPR171 RPS13 TSEN54 HLA-DRA CD52 AES PTGER2 COMMD8 EBP SYK LAT HSPE1 CYBA RPSA CHMP1B ACTB TC2N PSME2 TMUB1 NLRP3 NKG7 SAP18 EGR1 RNF149 HBEGF DYNLT3 RORA CD74 HLA-DQA1 CCL3L1 TRAT1 CCDC109B GZMM GAPDH IFI27 EIF3E CDK2AP2 CAPN12 STUB1 IL27 RARRES3 UBE2S SPINT2 SNRPD2 ATP6V1F OXNAD1 LAT C9orf78 CSNK1D ARHGDIB SERPINB6 CD97 POLR3GL HSPA1A TMSB10 SPINT2 GSTK1 PDLIM1 RPL14 VSIG4 COMMD6 PSENEN C9orf16 RALY ANXA2 HNRNPA1 LDHA GUK1 RPL22L1 VASP ACP5 EIF4A1 CCND2 FAM96B PPDPF RAP1A FUS GPR68 TOMM7 ARL5B RPSAP58 HNRNPUL1 TNFSF14 SNRPB2 MT-CYB EEF1A1 C14orf166 RHOC METTL5 GBP5 CREM SPINT2 IL16 RPL32 PSTPIP2 RCAN3 SURF4 SLC9A3R1 PNN GPR183 CD48 MZT2A MIF MBP HCAR2 SPOCK2 CXXC1 MT-CYB CLDND1 SAMHD1 TNFSF13B PCBP1 TTC1 GTF3A HAPLN3 EIF3H RPS18 SAT1 ATF6B CAPG SAT2 ANXA5 TSC22D4 CDC42SE2 EPSTI1 LYAR HMGN1 LAPTM4A ALG13 RNF130 PLP2 HCST SCML4 RPS16 ID3 MZT2A PSMA7 PTPN4 RBCK1 CREM MGAT4A LAPTM5 COMMD6 CD9 LITAF SMDT1 TIMP1 HLA-DRB5 CD74 CXCL3 ANXA5 EML4 RP11-47L3.1 PHGR1 PLA2G7 ENO1 AMICA1 SSNA1 EPSTI1 UBE2E2 TMEM14B ICAM3 CASP4 CD53 H2AFY PSME1 IL17A CTSB OAZ1 UBXN11 CYCS EIF1AX ARPC3 PPP1R18 RGS2 ATP5L DYNLT3 APRT RPS14 RHOG RBM3 IFITM2 RPL7 CSRNP1 CASP1 ICAM3 PRKCQ-AS1 VAMP8 BLVRB CD274 ALOX5AP RBL2 RPL4 RPL27 HCAR3 C19orf24 HSP90B1 HLA-DQB1 RPL3 LINC00936 GMFG SNRPB FAM173A OXNAD1 TUBA1B NEAT1 FERMT3 SLA2 NEDD8 IL18BP EGR1 GHITM GPR171 C11orf31 C12orf57 PTPRC SELT SAMSN1 HSPA9 EMG1 CD97 NFKBIA PSMB9 TPM3 PTGS2 UBE2D2 RPS16 CD37 CHMP4A MYO1F TXNIP RPL22L1 ANAPC16 PSENEN NADK GTF3A ISG20 RPL21 MLX RABAC1 RPS11 SNRPD2 RPSA RPL34 A2M PPP2R5C IFI35 HMOX2 CIB1 GDI2 SNRPG CASP1 LSM10 OCIAD2 GLIPR1 TMA7 NPC2 PSMD13 SLC38A1 HSPB1 RPL22L1 SLC1A5 PGK1 TADA3 DSTN IFITM2 TRAPPC1 TYROBP IDH2 NMI DUSP2 TUBA4A HLA-DRB1 GHITM CD9 RPL23 MAX C11orf48 NHP2L1 DUSP1 SCML4 UXT RPL28 ATP5D MCL1 C19orf53 HSPB1 GGA1 ACADVL BSG GGA1 RBM3 EEF1D ATP8A1 MT-ND3 MZB1 RAB8A LAPTM5 GATA3 RNF19B ARHGEF1 TAPBP GPR34 NAA50 GLIPR2 HERPUD1 RPL23A TSTA3 AKR1A1 PSMB9 JUN EMP3 BANF1 CD97 GAPT PHLDA1 UBA52 CDIP1 MZB1 NAGK PRKCQ-AS1 CRIP1 C11orf31 MEA1 C10orf54 ZFAS1 NR4A2 STXBP2 PSMB8 CTSB EEF2 TAP1 RPL22 MYEOV2 CD53 COTL1 SS18L2 CALM1 UBE2I CSF3R TRAPPC6A FLT3LG RPL36A ZFP36 SCIMP CTSD GPR183 NUDT14 FIBP MT-ND4 NDUFS5 IRF1 IRF2 C14orf166 PSMA4 CLIC1 CXCR3 MRPL46 SIGIRR HCST RPS24 PPP6C YPEL5 RPL10 Tregs Memory_T_cells NK_cells Cycling_CD8_cells Inflammatory_CD2_DCs IL32 LDHB NKG7 CD3D LST1 CORO1B RPL11 TYROBP CD3E IL4I1 BATF CCR7 FCER1G NKG7 KRT86 TIGIT RPS12 XCL2 CD2 LTB PFN1 RPL32 CTSW CCL5 FXYD5 BTG1 RPS3 XCL1 CD7 ALDOC CD3D RPL19 CLIC3 IL32 KRT81 ARHGDIB RPLP2 IL2RB GZMA ID2 CREM RPL13 GZMB CST3 LTA4H ICA1 RPS15A CCL4 ITM2A NFKBIA C9orf16 RPS14 GSTP1 TUBB4B ZFP36L1 DNPH1 RPL23A KLRC1 CTSW CASP3 TNFRSF4 RPL31 MATK PTPRCAP TNFRSF25 CARD16 RPSA APOBEC3G GZMB HSPA8 RAP1A RPS4X CST7 VIM MIR24-2 LTB RPL18 GZMA CD8A LIF ARPC1B RPS6 GNLY CD8B TYROBP CTLA4 RPS13 GZMK B2M DUSP1 NDUFV2 RPL28 CD7 CD96 NXT1 FOXP3 RPL27A KLRD1 AC092580.4 HNRNPA0 PMVK RPS2 HCST SH3BGRL3 MPG PBXIP1 RPS25 EIF3G CD3G HMGN3 LCK LTB PFN1 RGL4 CXCR4 CD63 RPS18 PRF1 LGALS1 NR4A1 BIRC3 RPL30 FGR FCGRT CSF2 PTPRCAP RPL4 KRT81 HCST PRMT10 ITM2C RPS9 HOPX PLA2G16 CD83 UCP2 RPL35A CAPG TMIGD2 DNAJA1 IL2RG RPS27A CCL3 IFNG H2AFY AC017002.1 RPS8 KLRF1 RAC2 SRSF2 SRGN RPL10A MAP3K8 GYPC TMIGD2 LGALS1 GNB2L1 SRGN SPINT2 OTUD5 CD44 CD63 IFITM2 LGALS4 CD300LF CALM3 RPS23 CD3D HLA-DRA SPINK2 DUSP4 RPS20 STK17A CD69 TPT1 RGS1 RPL14 FAM177A1 LY6E TLE1 TNFRSF1B RPL36 PTP4A1 LDHA DLL1 MIR4435-1HG RPL37 ITGB2 ARHGDIB PTGDR LAIR2 RPL13A CCL5 GIMAP7 NCOA7 ICOS IL32 BTG1 SRGN CD52 TNFRSF18 RPL27 NR4A2 TBC1D10C AMICA1 HLA-A PABPC1 APMAP CD52 MAFF ACTB RPL26 DUSP2 RPL8 BIRC3 SPOCK2 RPL8 PTGDR EPCAM JUNB ANKRD12 SELL GZMH RARRES3 TOX2 EIF3H RPS21 CORO1A CD9 DRAP1 GSTP1 RPL5 KRT86 H2AFZ CD69 B2M RPS15 CD160 ATPIF1 IL23R CORO1A RPL10 LAT2 MSN ARL4A CD27 LGALS1 ID2 APOBEC3G TCIRG1 CCL5 RPS16 MIB2 GZMM UBB LAT BTG1 ALOX5AP SLC9A3R1 IER2 PKM RPL34 BCO2 CDKN2A CAT PPP1R18 RPL29 NCR3 COX5B EIF1 ANXA1 RPL12 ARPC5L C15orf48 AREG EEF1D TMEM66 MYL12A ICAM3 FOSB HINT1 FXYD5 FTL TXN ZFP36 IL10 ARHGDIB CD97 CD37 TCP1 RAC2 RPS5 PPP1R2 SKAP1 CD164 ASB2 RPLP1 CD247 PIM1 DDX3X LAG3 RPS7 GLIPR2 SLA2 METTL9 FOS EEF1B2 CLIC1 TRAT1 ZNF75A ATP5L RPS19 SLC35E1 CXCR3 C16orf91 TBC1D4 CD52 7-Sep TCEA2 NR4A2 COTL1 FAU CHST12 PRKCH TNFRSF18 RPL28 RPL7A CDC42SE1 ATP5B MAP3K8 RHOH GLTSCR2 C20orf24 EMP3 TEX30 NINJ2 NOSIP LSP1 MARCKSL1 BZW1 RHOG NPM1 SAMD3 HLA-DRB1 H3F3B GMFG LEF1 PTPRCAP HLA-B DDX18 CST3 RPL6 HSPB1 PEBP1 MRPL18 CD52 ZFP36L2 ABHD17A TRAF3IP3 PRPF6 PPP1R2 RPL15 RGCC ATP5G1 PRAM1 UBE2D2 EIF3E CD44 RPL37A SLC43A2 FYB TCF7 MAPK1 HLA-DPB1 RAN TNFRSF9 HINT1 LDLRAD4 PRF1 FCER1G PTTG1 RPS29 ACTB HOPX MGAT4A CD2 RPLP0 EVL GSTP1 SLC25A39 TRAF3IP3 UBA52 TMIGD2 PDLIM7 NFKBIZ NTMT1 LEPROTL1 MRPL3 CST7 BLVRA RPS15A RPL22 GZMM GRN FOS ADTRP RPL38 ZFP36L2 HLA-DPA1 RNASET2 CACYBP ITM2C NUDT14 IFITM2 IL2RG S100A4 HSPA1A TESC LCK EIF4A1 GPR183 RPL3 SH2D1B EVL LINC00299 JUN TRAT1 CHD2 GZMK EMP3 ENO1 EEF1D FAM49B SIRPG DNAJB1 UBC EEF2 VDAC1 LGALS3 IL7R TNIP2 BTF3 BIN2 NANS BST2 1-Sep LGALS3 ARHGDIA CD74 CREM EVL SMDT1 CDHR1 CYC1 SLC16A3 CXCR6 PFDN5 SIGIRR AGR2 KIAA1324 HSPA8 TOMM7 VPS37B HLA-C UNC93B1 TAPSAR1 HNRNPA1 TNFRSF18 SH2D1A ENO1 GNB2L1 EIF3F GRK6 LAPTM5 SKIL XRCC6 CCDC109B DUSP1 SLC25A5 RNF139 CYTIP PTPRCAP ZFP36 CORO1A HSP90AA1 CD37 CD3D SELM HLA-A BEX2 RPL13A CD37 IDS HSPD1 TMEM243 NSA2 RPL23 PRDX1 RPL36 DDIT4 CD3E RPS3A RHOF IL2RB RBM39 HMGN1 PSAP LGALS3 LSP1 SIK1 TRAPPC4 GIMAP7 CFL1 TSPAN5 PSMD13 TRAPPC1 RPL24 CMC1 GCHFR RASD1 SH2D1A LIMD2 RNF113A ATP5G3 AQP3 TIMP1 RPL37A IL2RG HIST1H4C MED30 ARID5B RPL9 TIMM8B GPX2 HHEX SKAP1 RPS11 FASLG RPL38 ZNF331 DOK2 TRAF3IP3 TMSB4X SAMSN1 BTG2 SNRPB RPS24 SRSF5 COX5A RPL22L1 ISG20 PASK LAMTOR5 HN1 NCR3 TNFRSF14 TPT1 AKNA HLA-DQA1 MYADM FXYD5 NACA USF2 ATP5O LPXN CDKN2A CORO1A RAC2 UQCR10 RBPJ RPL36AL COX7C NDUFB8 UBE2C UBE2S PCBP1 IFITM3 SDHC GMFG DPAGT1 LAPTM5 EIF3H RANGRF GNG2 NHP2 PTPN2 CXCR4 KLRB1 FYN CYCS UXS1 ANAPC5 PSMB2 HES1 PRR5 PMAIP1 RPL18A SLC16A3 GNLY CCT4 UGP2 CD7 RIN3 ID2 HMGN1 9-Sep DENND2D RBM38 UQCRQ BCAS2 ARF6 MZT2A IDI1 XCL1 BTG1 CMC2 RPL35 UBXN2B HLA-DMA MAP2K1 LIMD2 FAIM3 LINC00667 RPS29 CXXC5 PSME1 OCIAD2 CST3 ANXA1 ATG4B LEPROTL1 GPSM3 PPP5C RGCC SFPQ TMSB4X C6orf48 ID3 CCNB1 SRGN IGBP1 UBB DRAP1 BST2 NPC2 PYHIN1 RNF138 NFKBIA ATP5A1 TUBA4A BCAS2 CYTH1 CCNL1 CLEC2D CALM1 PHLDA1 SERPINB6 NXT1 ECHS1 TXK PRR13 CCL5 ARID5A CCNB2 SPTLC2 ZNHIT1 FAM177A1 AGTRAP ATP5J2 ANP32A SOD1 DCXR ARHGDIB TNFRSF18 CCR6 MAPK1IP1L NUCB1 CBX3 CKS2 PROSC OSER1 DAP3 TCEB2 NCAPH TXNL1 CASP4 P4HB RPS3 RPL5 TRAF4 RGCC FYB ZNF814 RAC1 HSP90AB1 NAMPT HLA-DPA1 LINC00996 ARPC1B SRSF5 6-Sep FOSB PSMA7 ABI3 SLA IDI1 6-Sep CD69 GPX1 RNF19B GBP2 CHI3L2 YPEL3 MT1G COL9A2 SSU72 ID3 APRT CYTIP NFKB1 COPE CST3 HMGN1 SURF4 PPP2CA YWHAZ ARPC1B CPNE1 CTSH NAP1L1 COMMD3 JUNB IGFBP7 FXYD5 SRP9 GLRX RARRES3 PPP1CA PFKP BEX4 RBBP4 BEX2 YWHAZ CRIP1 TMEM123 PTPRC ICOS EBP ZAP70 TUBB4B HIGD2A HLA-DRB1 MIR24-2 ICOS LGALS3BP SMS IFITM1 ZNF331 MT1E TNF CCL20 PFN1 GCHFR RPL12 HSPD1 ANP32A CD3E TRAPPC1 RORA SAMD10 NPM1 TBC1D10C DDIT4 IL2RG CSTB NAPA RNASET2 GRB2 IFI16 CRIP1 APOE EIF2S3 OCIAD2 ETFB CD47 RPL15 CASP8 MPG UPP1 EMC10 HSPB11 FXN RALA ATP5J SACM1L ACTR3 CYLD C19orf25 S100A4 ANXA5 CDC42SE2 SC5D SNRPA1 PSMB9 IFI44L TMEM66 LMNA BUB3 STK17A CAPG SNX5 MAL PLAC8 RPS14 FAM213B CHCHD10 AIM1 PDCD4 KRT19 EIF3D ICAM3 TMSB4X SLC25A39 TIMM13 EIF4G2 JUNB MRPL16 RPL7L1 CD247 ERBB2IP LIMSI COTL1 NSMCE1 RPS4Y1 ARF1 EPSTI1 CRLF3 BUD31 RPL7A PARL C19orf43 H2AFV PAPOLA TMSB4X HSPA5 PIM2 AAK1 CALM1 RPS18 ZFAS1 LINC00152 SLC2A3 MRPS11 GZMH GSN GTF3C6 CTSD C1orf162 SRI WDR45B SOCS1 AC013264.2 PSME2 PIGR TPM3 RPL11 TMSB10 LDHB KRT18 SERTAD2 UFC1 1-Sep CD59 COX4I1 CA13 TSC22D1 IGBP1 RBCK1 CCL4 AKAP17A ARPC4 RPS4Y1 GRN CENPW CUTA NUDT1 ZFP36 BCAP31 STOM CDC42SE1 ANAPC16 COMMD6 AIM1 CREM PRKAR1A TPRKB DNMT1 TGFB1 PTTG1 EPS8L2 PHGR1 GIMAP4 TIPARP RPL35A H2AFX WDR1 CXCL14 MYO1F FKBP11 CXCL2 RPS2 YPEL5 SF3B2 PHB ALG13 CD58 WHSC1L1 NDUFS8 PTGER2 SNRPB DDX5 ZNF331 RTN3 SUCLG1 B3GALT5 RPS27A CD27 NDUFA3 ACAP1 NRBP1 SMCO4 GSTK1 PPP1R14B AIP AUP1 EEF2 SSU72 PTMA PLEKHF1 GPATCH3 LDHB HLA-DPB1 SH2D1A UQCR11 TRIAPI CUTA SPOCK2 PIGX HSPE1 SF1 TNIP1 TIMP1 PTPN4 TPM1 GPR65 SKP1 SLC25A6 JAK1 HINT1 VEZT ITM2A C1orf228 IRF8 DBI PCBP1 HCLS1 LCK TADA3 CCND3 NR1H2 HLA-G NAA38 HSPE1 ITK FKBP3 GYPC DCK GGA1 RPS6 TNFRSF4 RPS3 GPR18 RTCA CLDN7 CD3E SH3BGRL3 CTSC TLN1 CD53 GPR68 RPS27L HERPUD1 TRMT2A EEF2 TNFSF4 GPX1 TPI1 PSTPIP1 SH2D2A H2AFZ SNRPB2 RGCC GGNBP2 COX6B1 PSME1 AKIRIN2 LINC00861 NHP2 HMGA1 JMY PSMD8 CD59 PSD4 RNF187 NUP54 COX17 EVL RTFDC1 NDUFA11 XCL1 UBE2I CORO1B PSMD6 HMGN1 GNA15 SELT CYCS DCXR STMN1 LTC4S IL2RA ZNHIT3 TSPAN32 UQCRC2 TXNDC17 FAIM3 TOMM20 CUTC LAT GATA3 GK TUBA4A ATP6V1G1 HLA-DQB1 N4BP2L2 NAA38 9-Sep IFITM1 AK2 CTSH PSMA2 DGUOK C19orf66 WDR54 SLC39A4 SNRPD2 LYRM4 PPP1R18 RPS24 PER1 RPL24 FTL TMEM14C TSC22D3 AC022182.3 PIK3IP1 JUN ALKBH2 MTPN HCST ID3 LAT POLR2L MYO1G PCDH9 SLAMF1 PIK3IP1 METRNL KLRG1 TPI1 RPL18 OAZ2 SERBP1 NRM RP11-425D10.10 UBXN1 FOS C9orf16 FOSL2 SERTAD1 FTL HSPB1 BHLHE40 1-Sep KIT H2AFV AES TSC22D4 PRDX5 ERGIC3 CMTM7 COX4I1 S100A6 SSBP4 ZNF814 LINC00649 LRRFIP1 RBM39 RPS13 FOSL2 RPL34 RAB1A RNF125 GIMAP1 LYPLA2 HSD17B10 MALAT1 MAFF MPC2 SIVA1 BAX RILPL2 SLC9A3R1 COX7C JTB CLPP HLA-DRA STXBP2 GMNN ANP32E HSPA1B GTF3A CLDND1 GNB2L1 RNFT1 CD7 ABHD14B AP2M1 PABPC1 EIF5 RPS25 ACP5 PSMD8 HLA-DRB5 BAD HLA-DRA CHCHD7 VAPA FAM162A PNP ZNF706 RAN SOCS1 OASL HNRNPK RPL12 CD74 HNRNPA2B1 OSTF1 MGMT DCXR VAMP2 DHRS7 DOK2 TCTN3 CUL9 APRT AKIRIN2 C1QBP C6orf57 RNF213 C19orf43 COA5 LIMD2 PCNP ZC2HC1A TSC22D4 COMMD6 CD160 TP53I13 ALDOA BRMS1 ATG12 TUBB C3orf17 G3BP2 RASAL3 ARPC2 RPL24 MRPS15 HCST NDUFS6 KLHDC4 DDT GPX7 CIB1 NPC2 LRRFIP1 GTPBP1 CASP6 PDCL3 LSM14A APOBR ATP2B4 HLA-B SSBP1 CCDC104 ETF1 NDUFC1 CRTC2 CCT7 WDR82 CASP4 RAB27A MBOAT7 HPRT1 MEA1 CASP3 PRDX3 TNFAIP3 PTGES3 GADD45B CD53 CXCR6 DCAF11 MRPS35 ANXA2 U2AF1 RPL23 SRSF7 SRP19 CD28 TSEN15 CDC20 PPP1R11 HSP90B1 FCGRT AOAH NASP ZNF207 BUB3 LINC00649 HLA-DPA1 RHOF FURIN BTG3 PHGR1 OBFC1 CDKN3 WDR83OS

FIGS. 5 and 6 show that the cell composition changes between UC and healthy controls. Applicants can use the expression profiles to deconvolute bulk expression data. Thus, Applicants can determine the cell composition of a colonoscopy sample obtained from a subject and analyzed by RNA-seq.

Applicants also determined genes that were associated with disease. FIG. 7 shows genes differentially expressed across the entire colon and FIG. 8 shows genes differentially expressed in specific cell types. FIG. 9 shows differential gene expression in UC cell types for uninflamed and inflamed tissue. IL-32 and MHC-II are two of the strongest signals and are also genes identified by GWAS. Genes differentially expressed in each cell type during disease is shown in Table 2 A-F.

TABLE 2A NA 1-50 NA 51-100 NA 101-150 NA 151-200 NA 201-250 Plasma_B_cells Class_switching_B_cells MTRNR2L1 EMP1 TAGLN RPS29 MMP10 G0S2 TIMP1 HLA-B AKR1C1 TFF1 TMEM258 VSIG2 FABP1 RPL3 CHI3L1 CD63 HGF CLDN7 RAMP1 TNFRSF18 HSP90AA1 EIF5A FKBP1A PDIA3 PHLDA2 MT1M PHGR1 LMNA RPL3 PTMA CDH13 TMSB10 APOA4 AGR2 ILVBL S100P COL6A3 ACADS F2R TFPI2 GAS6 CD69 TIMP1 REG3A KDELR2 PXMP2 FXYD3 RPL3 CTHRC1 REG1A BACE2 NOP10 SRM MORF4L1 LMNA TNFRSF4 C8orf4 C10orf99 SELM CFB PEBP1 TIMP1 G0S2 HMGCS2 CNN3 HAPLN3 NDUFA4L2 STAP2 SMOC1 PABPC4 DMBT1 CEBPB FABP4 CBX3 NFKBIA HIST1H1C ITM2C AC005540.3 RPL13A PTGES NXPE4 MT-CO3 HSP90AA1 AGR2 OLFM4 LCN2 DSTN ACAA2 DHRS11 TNFRSF4 RPS3A IL13RA2 HSPA1B CCL5 NDRG2 SPINT2 HSPA1A RNASE6 MMP3 CKB VAMP8 KANSL1-AS1 PRRX2 HSPA1B LGALS4 REG4 PHGR1 MT-ND1 KLF2 RCN3 CYP20A1 HLA-DMA IGJ CD59 SERPINH1 LAPTM4A EIF4A1 KRT19 FXYD3 DEFA5 C11orf96 HYI ITGA5 TUBB CXCR4 PTMA TNFRSF12A ANXA5 POLR2L DHRS4 TSHZ2 DNAJB1 TNFRSF18 BGN RPL18A PPIB CDX2 KRT8 XBP1 RP11-16E12.2 SELENBP1 COL4A1 HLA-DMA PRKCDBP ACTN1 GOLGA2 H3F3B TPM4 CTHRC1 TST RPL6 VAMP5 CADM1 KLF6 IFITM2 PCOLCE AQP1 SOCS3 RPL10 NA QPRT TNFRSF11B COL1A1 SPARC GPR160 IL11 NA TPM4 PKM FTL CA2 PPDPF AGT NA SMOC1 PHLDA1 EMP3 CCL13 SEPP1 SERPINA1 NA NA MT1G GEM MT-CYB TMEM141 SLC26A2 NA NA LGALS4 COL4A2 HLA-DPB1 ELP5 CLU NA NA IGFBP5 PRSS23 SPINK1 NRG1 APOBEC3B NA NA URAD S100A6 AQP8 SPON2 DNAJB1 NA NA ANXA2 S100A3 ATOX1 CXCL1 THBS2 NA NA HLA-DRA CA1 RPL37A ID3 UBD NA NA PLA2G2A REG1B IER3 PTRF PIM3 NA NA PDPN TNC ENO1 CALR PRKAR1A NA NA S100A11 CCR7 MT1H TMEM165 IL32 NA NA SELL MEOX1 HSPA5 HSP90B1 IGFBP7 NA NA SOD2 FGF7 HSPA1A CLEC9A UGT2A3 NA NA LDHA MMP1 ITM2C INHBA HLA-DRB5 NA NA SMDT1 RPS3A SDC2 SPHK1 PPA1 NA NA CCL8 THY1 ID1 FABP1 CHCHD10 NA NA FCGRT RPS26 AMN LGALS2 COL6A2 NA NA RPL9 PKIB FABP6 PDLIM4 CD55 NA NA CYR61 CHP2 PIGZ TMEM158 RNASET2 NA NA NNMT SERPINE1 COL8A1 CKMT1A CTGF NA NA LMNA TXNIP DUOXA2 TRMT112 MT-CO1 NA NA HIF1A COL6A1 TPM2 CCDC3 CTSK NA NA CD82 RPS4Y1 CRIP2 HOXB13 C19orf10 NA NA LINC00152 PSME2 HYAL2 MRGPRF SERPINE2 NA NA TAGLN2 CAV1 CPXM1 CALU HSD17B12 NA NA IFITM3 ANGPTL2 NCOA7 ACSF2 SAA1 NA NA Follicular_B_cells 1-50 Follicular_B_cells 51-87 Microvascular_cells C12orf75 LTB PLAT METAP2 CLIC4 AQP1 CCND3 LSM10 CD9 HLA-DQB1 GDI2 HLA-A HLA-DRB5 RGS16 HLA-DRA RPS4Y1 CAPG EGLN3 TUBB2A SRSF2 LDHB LCK ZFAND2A HLA-C RMI2 RPL36 RBP5 SMARCB1 CBX3 CD99 HLA-DPB1 AGR2 PASK TCEA1 MRPL47 S100A10 MME TRA2A SERPINE1 RPL9 FBL CXCL12 SLBP SELT JUN CD63 SUMO2 ANXA2 UBE2D3 HADHB TESC A4GALT DEF8 IGJ PLD4 FGD2 FOSB SIT1 LIMD2 LIMS1 PPP1CC PSIP1 HSPA1A PAIP2 RBBP7 CALU CCDC109B BZW1 RCN3 DCAF12 TSTD1 S100A6 SRSF3 MTF2 CST3 HLA-DQA1 IKZF1 PRSS23 HLA-C RUVBL1 SEPP1 ISG20 BACH2 HSPA1B HMGN1 PIM1 WWTR1 HMCES CHRAC1 RAMP1 HNRNPC EZR GPX4 HLA-DPA1 MCM5 PSMB9 TUBB2B IGJ PSME2 HNRNPA3 COX6B1 CTGF CD27 PRPSAP2 CD82 EIF1AY TK1 LGALS4 ITGAE CCR7 SNED1 TPD52 TNFRSF4 ECHS1 IER3 RAP1B VAMP8 HLA-DQA2 ALDOA GGA2 HLA-B CHCHD10 TAP1 ACTR3 CD36 HLA-DRA F2RL3 SGPP1 KDR PGAM1 COL15A1 DCK PLAU TSG101 NA HNRNPM NA

TABLE 2B Post-capillary_venules Vitamin_metabolizing Endothelial_pericytes Enterocytes Tuft_cells PTGS1 PLAT FAM222B SPINK1 PTGS1 RAMP1 CXCL12 RP11-490M8.1 PLA2G2A ESYT2 PDLIM1 ENPP2 TWF2 IL18 SHC1 HLA-A TXNIP ZNF205 ATP1B3 HPGDS OLFML3 IGFBP4 HYI MTRNR2L1 HOOK1 PLAT CD36 NA GSTP1 BCKDK STXBP6 ANXA2 NA GPX2 RALGAPA1 UBD OAZ2 NA CYBA NA LY6E CD320 NA TAX1BP3 NA TNFSF10 AQP1 NA S100A14 NA CD9 CTGF NA NQO1 NA MGP RGS5 NA TSPAN3 NA CPE TGFBR2 NA NAALADL1 NA PSMB8 RAMP1 NA CTSA NA PHLDA1 CD9 NA RARRES3 NA EIF4A2 C16orf80 NA OAS1 NA GIMAP7 CXCR4 NA LGALS1 NA TMEM100 CLDN5 NA HMGCS2 NA CST3 STC1 NA PCK1 NA HLA-C GJA1 NA PRDX5 NA RPL9 FAM213A NA MUC1 NA RPL10 PLAU NA TMEM37 NA LPCAT4 HLA-E NA KRTCAP3 NA AQP1 PRKCDBP NA MT2A NA GIMAP1 RBP5 NA MX1 NA SRPX RPL9 NA S100A11 NA MALAT1 SAT1 NA NA NA RPL3 TNFSF10 NA NA NA AGR2 S100A4 NA NA NA PRSS23 TSPAN7 NA NA NA COL4A3BP AKR1C3 NA NA NA EFEMP1 C8orf4 NA NA NA SNHG7 HLA-DPB1 NA NA NA TUBA1B SRP14 NA NA NA PTGES TNFRSF4 NA NA NA NFKBIZ TIMP1 NA NA NA B2M ANXA1 NA NA NA FTH1 C1orf54 NA NA NA C19orf66 RND1 NA NA NA CDKN3 ANGPT2 NA NA NA RNF181 EGR1 NA NA NA EEF1B2 STAT3 NA NA NA MDK SH3BP5 NA NA NA CLIC1 RPL29 NA NA NA TPTEP1 CTNNBIP1 NA NA NA TFF3 LSMD1 NA NA NA S100A10 HLA-C NA NA NA JUN RBM17 NA NA NA CRIP1 GYPC NA NA NA MED24 NDUFA7 NA NA NA NA IER2 NA NA NA NA COTL1 NA NA NA NA RPLP0 NA NA NA NA SDPR NA NA NA NA IDI1 NA NA NA NA SLC6A6 NA NA NA NA RPL10A NA NA NA NA MYL6 NA NA NA NA AQP3 NA NA NA NA NKX2-3 NA NA NA NA COASY NA NA NA NA SOD2 NA NA NA Goblet_2 Absorptive_TA_1 Secretory_TA Absorptive_TA_2 Cycling_TA SPINK4 REG1A HLA-DRA AGR2 RARRES2 NUPR1 CD74 HLA-DRB1 HLA-DRA ARHGDIB S100A14 RPL3 RARRES2 CD74 IGJ BAIAP2L1 HLA-DRB1 ID3 S100A11 BST2 BDKRBI MT2A HLA-DMA HSPB1 PKIG MT-ND2 RPS3A UGT2B17 SPINK1 PITX1 FAM3B ARHGDIB CD74 HLA-DRB1 ETS2 MUC13 TIMP1 HLA-DRB5 TIMP1 HLA-DRA TFF1 LIN7C REG1A RARRES3 TIMP1 ANO9 MTRNR2L1 HLA-DPB1 SELENBP1 MTRNR2L1 TUBB2A KCNK6 HLA-DPA1 GPX2 HRCT1 NA RPL18A GLB1L2 MUC12 ZNF90 NA TNFRSF12A NA ID3 MUC12 NA SEC11C NA ARHGDIB AKR1B1 NA NA NA REG1A HLA-DPA1 NA NA NA PLA2G2A VAMP7 NA NA NA CEACAM5 S100P NA NA NA IDH2 NQO1 NA NA NA IGJ DEK NA NA NA RNASET2 ABRACL NA NA NA BSG REG1A NA NA NA PSMB9 ACAT1 NA NA NA ADIRF DNAJB1 NA NA NA LEFTY1 HLA-DRB1 NA NA NA RARRES1 IGFBP4 NA NA NA LYZ NA NA NA NA MTRNR2L1 NA NA NA NA TFF1 NA NA NA NA RPS4Y1 NA NA NA NA SRSF6 NA NA NA NA CNPY2 NA NA NA NA GSTP1 NA NA NA NA ATP1B3 NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA

TABLE 2C Goblet_1 Stem_cells Enteroendocrine Glial-cells Inflammatory-fibroblasts Fibroblast_pericytes SPINK4 AQP1 RARRES2 ALDH1A1 COL1A2 NET1 ITLN1 RPL3 HLA-DRA CLU GBP1 NA IGJ RPS4Y1 SEC11C ANXA1 IFI27 NA AGR2 LYZ MT2A SPP1 DYNLT1 NA SDF2L1 LCN2 NIPSNAP1 IL32 PKM NA TIMP1 ID3 OLFM4 CAPS PHLDA1 NA PDLIM1 HLA-DRA DDC FIBIN DUSP1 NA MUC2 HLA-DRB1 MDK RPL3 CNOT4 NA LYZ HLA-DMA CD82 RPL9 CCL8 NA SELK HLA-DPA1 NA HLA-G LAP3 NA HMGCS2 C2 NA MRPS6 ACP5 NA SEC11C NQO1 NA LINC00152 GSTT1 NA SSR4 B2M NA HOXC6 GALNT11 NA DNAJA1 ARHGDIB NA CDKN2A PSMB9 NA FKBP11 DNAJB1 NA TUBA1A TNIP2 NA REG4 RARRES2 NA HLA-DQA2 PSMB8 NA EZR MTRNR2L1 NA SOCS3 HAPLN3 NA SELM HLA-C NA SEPP1 PERP NA CISD1 CD74 NA IGJ NA NA SYTL1 C19orf70 NA HLA-DRB5 NA NA PHLDA2 GSTT1 NA KLC1 NA NA CHPF TESC NA HLA-DRB1 NA NA NA IFI27 NA NDUFB4 NA NA NA PSME1 NA ENTPD2 NA NA NA HMGCS2 NA SRGN NA NA NA HLA-DRB5 NA PMEPA1 NA NA NA RPL6 NA HSPA1B NA NA NA UGT2B17 NA FKBP1A NA NA NA HLA-DPB1 NA GLIPR2 NA NA NA PSMB9 NA UBR4 NA NA NA SCARB2 NA UBB NA NA NA NA NA COX7A1 NA NA NA NA NA LSM3 NA NA NA NA NA PRDX2 NA NA NA NA NA NUPR1 NA NA NA NA NA NA NA NA Myofibroblasts Villus_fibroblasts Crypt_fibroblasts_(hiFos) Crypt_fibroblasts_(loFos) PDLIM7 MMP2 TM4SF1 GPX3 NBL1 SRPX2 VASN NR4A1 C12orf75 TNC GSN C1S PHLDA2 MMP1 FGF7 TM4SF1 IGFBP5 S100A4 PLAT DUSP1 PRSS23 NSG1 CLEC14A ID1 TM4SF1 EDNRB IQGAP2 LGALS3BP SQRDL AGT ID3 COL15A1 MRGPRF TRPA1 FN1 SERPING1 RERG CPE SEPP1 TNFAIP6 MXRA8 VSTM2A TNXB CFD RPS4Y1 RBP4 CCL13 ADAMDEC1 EGR1 TSHZ2 TPBG MZT2B HOXD9 IL32 HSD17B2 MIF TDO2 VASN STMN2 EGR1 DUSP1 CRIP1 GPX3 DKK3 LMNA NR4A2 VIM NBEAL1 CYB5R3 PCTP TNFSF10 GSN DDAH2 PRSS23 NA GGT5 TFPI2 MCL1 NA FOXF1 NA NDUFA4L2 NA RPL9 NA ANXA1 NA CD74 NA TMSB4X NA NA NA PDLIM1 NA NA NA IGFBP3 NA NA NA CEBPD NA NA NA FOXF1 NA NA NA ACP1 NA NA NA C1S NA NA NA FRZB NA NA NA ECM1 NA NA NA DMKN NA NA NA ID4 NA NA NA PDGFRA NA NA NA GADD45B NA NA NA SPARCL1 NA NA

TABLE 2D T_cells Macrophages Dendritic_cells Mast_cells Cyding_monocytes Tolerogenic_DCs NUB1 LGMN CST3 NFKBIZ TFF3 TXN CAV1 RNASE1 MARCKSL1 EGR3 ATP2A3 NA EIF2S1 AKR1B1 CD52 IL1RL1 GSDMD NA COL6A1 LGALS2 PPA1 HLA-B EMP3 NA POSTN A2M IGJ CAPG IL12RB1 NA ALAS1 C15orf48 SERPINB1 EGR2 PSMD11 NA RGCC VMO1 TYMP HLA-C ENPP2 NA NA SERPINF1 STMN1 RPS4Y1 ALOX5AP NA NA SPINT1 FCER1A CTSW AK1 NA NA ACP5 DNAJB1 EIF4G2 NA NA NA TFF3 PRELID1 ZEB2 NA NA NA RNASET2 NA NA NA NA NA ENPP2 NA NA NA NA NA LGALS1 NA NA NA NA NA MMP9 NA NA NA NA NA CORO1A NA NA NA NA NA CSTB NA NA NA NA NA SELK NA NA NA NA NA MT2A NA NA NA NA NA FBP1 NA NA NA NA NA PLSCR1 NA NA NA NA NA FXYD5 NA NA NA NA NA NR1H3 NA NA NA NA NA UCHL3 NA NA NA NA NA SEPP1 NA NA NA NA NA AGR2 NA NA NA NA Neutrophils Activated_CD4_cells_loFos Activated_CD4_cells_hiFos CD8_IELs GBP1 S100A4 IGJ CCL3 FCGR2B RPS29 ADSS CCL4 GSTO1 TIMP1 NA RPL10 RPL30 RPL9 NA RPL6 TMEM176B CFL1 NA CD3E EMG1 VIM NA MTRNR2L1 GDI2 ANXA1 NA ARHGDIB NA PHLDA1 NA CD3G NA S100A11 NA RPL3 NA HLA-A NA ITGB2 NA NA NA KLRB1 NA NA NA IFNG NA NA NA RPL22 NA NA NA RPL18A NA NA NA PTMA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA NA

TABLE 2E CD8_LP_cells Tregs Memory_T_cells NK_cells Cycling_CD8_cells RPL9 CD7 RPL9 ILF3 ENTPD1 EMP3 CD2 PFN1 CALCOCO2 CD2 ARFRP1 TIA1 IL32 CD47 EIF5A NA GRSF1 ANXA1 NA LCK NA NA S100A4 NA HAVCR2 NA NA ARPC1B NA ATP5L NA NA KLRB1 NA KLRB1 NA NA RPL30 NA CALR NA NA ANAPC5 NA MTPN NA NA GAPDH NA CENPA NA NA B2M NA MIF NA NA RPS28 NA NA NA NA PSME2 NA NA NA NA AK5 NA NA NA NA SERF2 NA NA NA NA RILPL2 NA NA NA NA RPS29 NA NA NA NA TAGLN2 NA NA NA NA FXYD5 NA NA NA NA S100A11 NA NA NA NA ANXA5 NA NA NA NA S100A6 NA NA NA NA PNRC1 NA NA NA NA ARPC2 NA NA NA NA ZFP36 NA NA

Applicants were able to determine the cell of origin for genes associated with disease by genome wide association (GWAS) (e.g., IBD). Previous studies have shown 94 IBD loci fine mapped in 67,852 individuals (Hung et al., Nature 2017). FIGS. 10 and 11 show violin plots for key IBD genes in healthy and disease samples. Applicants also show heatmaps for GWAS genes expressed in each cell type (FIGS. 12 and 13). Applicants show a heatmap for G-protein coupled receptors (GPCR), genes involved in cell-cell interactions, and in epithelial cells in the gut cell types. (FIGS. 14, 15 and 16). Key genes are highlighted in FIG. 16. FIG. 17 shows that genes associated with other disease indications can be localized to specific cell types in the atlas.

Applicants also show that the atlas may be used to determine cell-cell interaction mechanisms within the gut (FIG. 18). FIG. 19 shows cell-cell interactions in healthy tissue and FIG. 20 shows cell-cell interactions in diseased tissue. Applicants identified for the first time cell types that interact in healthy and disease gut tissue and have determined high specificity ligand receptor pairs that allow the cells to interact. Not being bound by a theory, modulating these interactions can allow modulation of the gut to prevent and treat disease (e.g., IBD). Not being bound by a theory the interactions may be disrupted using small molecules, antibodies and/or soluble proteins.

Finally, Applicants show that fibroblasts that support the stem cell niche can be identified using the atlas (FIGS. 21-24). FIG. 22 shows genes expressed in the villus (e.g., BMP) and genes expressed in the crypt (e.g., Wnt). Genes associated with either locus can be identified by examining gene expression the tSNE plot. For example, FIGS. 23 and 24 show RSPO3 expression in the tSNE plot and an RSPO3 module may be identified by co-expression in the plot (e.g., MGP, C7, GUCY1A3, TNFSF13B, CXCL12, C3, and C1QTNF3).

The genes and cell types identified in this study can also be used to perform in situ validation, functional tests (e.g., organoids), GWAS covariation studies (e.g., to relate changes in cell types through molecular connections).

Example 2scRNA-Seq Atlas of Colon Biopsies from Healthy Individuals and Ulcerative Colitis (UC) Patients

To understand the cellular and molecular changes associated with UC, Applicants obtained 115,517 high-quality single cell transcriptomes from 34 colon biopsies (each <2.4 mm²) that were collected from 7 patients with left-sided colitis and 10 healthy individuals who underwent colonoscopic examination (FIG. 25, STAR Methods). To investigate the transitions between healthy mucosa and chronic inflammation, while mitigating patient-specific variability, paired samples were collected from each subject during a single procedure. For UC patients, these were assessed as adjacent inflamed and non-inflamed tissue (FIG. 25, STAR Methods); non-inflamed biopsies may be either “non-colitis” (i.e. no history of inflammation) or “post-colitis” (i.e. resolved inflammation). From healthy subjects, these were two location-matched adjacent samples to estimate transcriptional and compositional variability. Immediately after collection, Applicants separated tissue samples into “epithelial” (EPI) and “lamina propria” (LP) fractions (allowing recovery of sufficient LP cells), dissociated them into single cell suspensions, and profiled the cells using scRNA-seq (FIG. 25 and FIG. 31, STAR Methods). As expected, EPI samples mostly consisted of epithelial cells (89%±15% epithelial cells on average) with some tissue-resident immune cells, such as intraepithelial lymphocytes and mast cells (FIG. 26D), whereas LP samples primarily contained immune and stromal cells (84%±18% immune and stromal cells on average).

Example 3—a Comprehensive Census of 51 Cell Subsets and their Molecular Signatures

To construct a cell atlas of the human colon in health and disease, Applicants used the expression levels of known markers to divide the cells into three groups: i) epithelial cells, ii) immune cells, including myeloid and lymphoid lineages, and iii) stromal cells, including fibroblasts, glia, and endothelial cells.

The single cell profiles partitioned into 51 subsets by unsupervised clustering (FIG. 26B,H, after correction for technical and biological variation, STAR Methods), which Applicants annotated post-hoc known markers (FIG. 26C) to reveal 15 epithelial, 23 immune (lymphoid and myeloid) and 13 stromal (fibroblasts, glia, and endothelial cells) subsets. The “cell subsets” almost invariably had representation from all specimens, and were proportionally distributed across samples of the same type (FIGS. 26D and 31), indicating that the clustering is driven by shared programs across samples, rather than by inter-sample differences.

Even though the cells were isolated from miniscule biopsies (˜2.4 mm²), the 51 subsets recapitulate nearly all of the known cellular diversity within the colonic mucosa (FIG. 26B) and highlight new subsets (below). This includes 15 subsets of epithelial cells, pseudo=temporally ordered along the differentiation trajectory (FIG. 26H), from LGR5⁺ intestinal stem cell to mature absorptive and secretory cell fates and including M cells (below); 8 subsets of fibroblasts partitioned defined by WNT and BMP signaling, including novel inflammation-associated fibroblasts, discussed below (also, including three subsets of WNT2B+ fibroblasts, two subsets of BMP4+ fibroblasts, as well as RSPO3+ fibroblasts, myofibroblasts, and inflammation-associated fibroblasts); four subsets of endothelial cells partitioned; one glia subset; seven myeloid cells (including inflammatory monocytes; below), four B cell subsets, ten T cell subsets across CD4⁺ Tconv, CD4⁺ Tregs and CD8⁺ cells, including CD8⁺IL-17⁺ T cells, and CD4⁺PD-1⁺ T cells, innate lymphoid cells (a mix of ILC2s and 3s), and NK cells (NKs) (FIG. 26B,H). To Applicants knowledge, known subsets missing from the census include submucosal enteric neurons, which require a distinct isolation approach (e.g., single nucleus RNA-Seq Habib et al., 2017), plasmacytoid dendritic cells (pDCs; possibly due to either low frequencies or uneven spatial distribution), and neutrophils, which express degradative enzymes that may damage their RNA or membranes. As expected, Applicants do not capture submucosal cells, such as myocytes and adipocytes, which require colon resection material.

Each cell subset is supported by a distinct expression profile, including known and new markers of known subsets and signatures of new subsets (FIG. 26H), with cell type-specific transcription factors (TFs), G protein-coupled receptors (GPCRs), transporters, cytokines, and pattern recognition receptors (FIGS. 32-36). For example, the CD4⁺FOXP3⁺IL10⁺ T_(regs) expressed BATF, a critical TF for the differentiation of tissue-resident Tegs (FIG. 32); inflammatory monocytes, thought to underlie chronic immune activation in many diseases, but not previously profiled in UC patients, express Oncostatin M (OSM), a cytokine associated with resistance to anti-tumor necrosis factor (TNF) therapy in IBD patients (FIG. 35). Surprisingly, compared to other cell types, plasma cells and cycling B cells expressed relatively high levels of the NOD-like receptor, NLRP7, a gene associated with IBD through GWAS, which recognizes microbial lipopeptides and is not known to be expressed by B cells (FIG. 33).

Example 4—New BEST4⁺ Epithelial Cells and Fibroblast Subsets in the Healthy Colon

The census reveled a new subset of chemosensory BEST4⁺ enterocytes that express genes related to acid and electrolyte sensing (e.g., pH (acid sensing) and electrolyte balance) (FIG. 26E), including BEST4, OTOP2, CA7, and Renin (REN), to likely complete a local renin-angiotensin system (RAS) in the colon (FIG. 26E,G). In particular, the otopetrin family encodes proton-selective ion channels, including OTOP1, which is enriched in taste receptor cells and contributes to sour taste perception through the detection of acids. Within the intestine, tuft cells are thought to transduce bitter, sweet, and umami tastes through the calcium channel TRPM5, but distinct pathways are required for sour and salty tastes. BEST4⁺ enterocytes may therefore be responsible for pH sensing and sour taste perception within the colon. These cells also express SPIB, a TF also expressed by tuft and microfold cells, suggesting they may be developmentally related. Based on the data (FIG. 26G), angiotensinogen is produced by WNT5B fibroblasts, renin by BEST4⁺ enterocytes (e.g., in response to local electrolyte levels), Angiotensin Converting Enzyme (ACE) by epithelial and endothelial cells, and the angiotensin receptor AGTR1 by WNT2B⁺ fibroblasts and pericytes, suggesting this pathway may be involved in local colon vasoconstriction.

Multiple fibroblast subsets differed by the expression of WNT and BMP signaling genes, reflecting distinct positions along the intestinal crypt-villus axis. One subset is transcriptionally similar to subepithelial telocytes, a rare population of mesenchymal cells that supports the epithelium that were recently profiled in mice. Some express higher levels of WNT2B, WNT4, and DKK3, and thus may reside near the intestinal crypt, whereas others highly express BMP4, BMP5, and WNT5, and thus may reside away from the crypt (FIG. 26F). All subsets express low levels of FOXL1, the defining marker of subepithelial telocytes in mice, a rare population of mesenchymal cells that supports the epithelium, and share additional marker genes with subepithelial telocytes, but the data show that these genes have distinct expression patterns in humans (FIG. 26F). WNT5B subsets (but not Tuft cells) are major sources of expression of thymic stromal lymphopoietin (TSLP), a cytokine that is crucial for the activation of ILC2s and Th2-inducing DCs in the colon, and of the receptor for glucagon-like peptide 2 (GLP2R), a peptide hormone produced by enteroendocrine cells to regulate gut metabolism and physiology (FIG. 26F).

One subset of WNT2B fibroblasts expresses R-spondin-3 (RSPO3) (FIG. 26E,F), the ligand for LGR5, a hallmark receptor of ISCs This subset expresses several other genes related to WNT/BMP signaling, including Gremlin 2 (a BMP inhibitor), glypican, and secreted frizzled-related protein, along with the immune recruiting chemokines CCL11, CCL19, CCL21, and CXCL12 (also expressed by secondary lymphoid organs), supporting a role of an inflammatory microenvironment to maintain the ISC niche.

Example 5—the Colon Cellular Composition in Dramatically Remodeled in UC

Changes in the composition of cell types that monitor luminal contents and titrate the immune response may affect the functional integrity of the mucosa in UC. To identify such changes, Applicants searched for cell subsets whose proportion changes in the colon between healthy, non-inflamed, and inflamed specimens. Prior work has examined changes in specific cell types, such as infiltration of neutrophils, mast cells, and IL-17⁺ T cells into the LP, but typically focused on specific cell types. Conversely, the census captures an extensive range of cells simultaneously, but, by definition, as the frequency of one cell subset increases, the frequencies of others decline. Thus, Applicants tested for changes in each subset proportions with a conservative statistical model that accounts for these dependencies (STAR Methods). (To identify changes that may be statistically dependent but physiologically important, Applicants also performed univariate analysis; FIG. 29E)).

The analysis highlighted a dramatic remodeling of the colon's cell type composition, spanning 9 epithelial subsets, 10 immune subsets and 9 stromal subsets. often with gradual changes from healthy to uninflamed to inflamed tissue. Applicants correctly captured many changes in cell proportions in UC patients that were previously reported, such as the increase in non-inflamed and inflamed samples in proportions of gut resident mast cells, CD8⁺IL-17⁺ T cells, T_(regs), and endothelial cell subsets in non-inflamed and inflamed samples (FIG. 27A). The magnitudes of these changes increased progressively from healthy to non-inflamed to inflamed samples, suggesting that even nominally “healthy” tissue from UC patients is altered and may represent a transitional state along the course of disease (pre-inflammation or post-resolution).

Although the total number of immune cells increased with the disease, within the immune compartment, colitis was associated with substantial reductions in plasma B cells and proportional increases in FO B cells (FIG. 27A). Within plasma cells, the frequency of IgA⁺ cells decreased and that of IgG⁺ cells concomitantly increased in both non-inflamed and inflamed tissue (Spearman's p=−0.80; P=1.4×10⁻⁷; FIG. 38), suggesting that immunoglobulin class-switching is occurring in the cells and may promote tissue inflammation and the generation of auto-antibodies.

Consistent with studies of inflammation in mice, microfold cells (M cells), specialized follicle associated epithelium (FAE) cells that deliver luminal antigens to immune cells situated in their basolateral pockets, were rarely found in healthy patients, but expanded significantly with UC (FIG. 27A). M cells play major roles in recognizing the gut microbiota and initiating mucosal immune responses. They highly express chemokines such as CCL20 and CCL23 suggesting that increased antigen sampling from the lumen is coupled to immune cell recruitment at the site of inflammation. Their expansion outside of lymphoid follicles with UC is unexpected, although congruent with studies of inflammation in mice, and suggests that M cells may have previously unappreciated roles in the disease.

Example 6—a New Inflammation-Associated Fibroblast Subset Unique to the UC Colon

Although most fibroblast subsets are present in both healthy subjects and UC patients, Applicants discovered a new subset of fibroblasts found almost exclusively within biopsies from UC patients, particularly in inflamed samples (FIGS. 26D and 27A), which Applicants termed colitis-associated inflammatory fibroblasts (CAIFs). CAIFs are enriched for the expression of fibrinolytic enzymes (e.g., MMP3, MMP10, PLAU) and immune signaling molecules (e.g., IL1R1, IL13RA2, CXCL6, CCL11, TNFSF11, TNFRSF11B) (FIG. 26E). In particular, IL13RA2 is a decoy receptor with high affinity for IL-13, suggesting that these cells may reinforce inflammation by neutralizing IL-13. Consistent with this hypothesis, deletion of IL13RA2 led to attenuated colitis in mice treated with dextran sodium sulfate (DSS). CAIFs also express high levels of chitinase 3-like-1 (CHI3L1), a biomarker of chronic inflammation and IBD-associated colonic dysplasia that is also associated with increased cancer-related mortality. CHI3L1 and IL13RA2 are known binding partners that can activate downstream MAPK and Akt signaling, and CAIFs have the greatest mean expression of the PI3K-Akt signaling pathway across all cell subsets (p<10⁻⁶ in all comparisons, Mann-Whitney test). CAIFs are also enriched for WNT2, one of the most upregulated genes in the intestinal stroma of colorectal cancer patients relative to healthy controls.

Example 7—Shift in Goblet Cell Differentiation May Explain Mucosal Changes in UC

Defects in the mucus layer in UC patients is a diagnostic feature and is widely attributed to goblet cell mucin depletion. However, Applicants generally did not observe cell-intrinsic reductions in mucin gene expression, suggesting that these defects may arise from degradation of the mucus layer or changes in the proportions of mucus-producing cells. While Applicants observed no significant changes in the frequencies of mature goblet cells, inflamed biopsies from UC patients showed a loss of goblet cell progenitors (FIG. 27A), coincident with a reduction in epithelial “stemness.” In particular, along the continuum of epithelial cell differentiation (FIGS. 26H and 27B), there were significantly reduced proportions of secretory progenitor cells (p<10⁻⁴; likelihood ratio test on fixed effect in mixed linear model; STAR Methods), in inflamed samples of UC patients. Defects in the mucus layer may therefore be explained by reduction in goblet cell progenitors. Interestingly, these cells are major sources of antimicrobial peptides, including REG4, ITLN1, and RETNLB, and may therefore correspond to the “deep crypt secretory cells” that help maintain the colon ISC niche.

Example 8—Most Cell-Intrinsic Expression Changes in UC are Shared Between Inflamed and Uninflamed Regions

Intestinal pathology during colitis is likely driven both by alterations in tissue composition and by changes in cell-intrinsic cellular programs. To explore the contribution of cell-intrinsic changes, Applicants modeled the expression of each gene as the sum of distinct components, reflecting cell subset, disease state (healthy, non-inflamed, or inflamed) and technical confounders, as well as correction for ambient RNA contamination in droplets (Macosko et al.) (STAR Methods). Fitting this model at different levels of the cell lineage, Applicants distinguished between general expression changes that are shared across an entire compartment (epithelial, stromal, immune, FIG. 27C-E) and unique changes within each subset (e.g. M cells, CAIFs, CD8⁺IL-17⁺ T cells) (FIG. 27F-H, Tables 3-9, 11 and 12, STAR Methods).

Despite being collected from grossly normal tissue, non-inflamed specimens shared much of the differential expression (DE) signature of inflamed tissue (FIG. 39A-F, Table 13-15), suggesting that the transcriptional signature of the disease may precede inflammation or persist after it resolved. Applicants therefore first focused on this shared signature, and then examined the minority of genes that were unique to inflamed tissue during active disease. (Applicants note that for the cell types which are nearly undetectable in healthy tissue, such as CAIFs and M cells, Applicants cannot robustly assess differential expression vs. healthy tissue).

Within epithelial cells, expression changes largely reflect the attempt of the disrupted epithelial barrier to regain tissue homeostasis by activating mucosoal immune responses, anti-microbial defenses, tissue repair and antioxidant defense pathways, biosynthesis of O-glycans and alternative mucins (FIG. 27C), consistent with the remodeling of the mucosal environment, as well as the MHC class II machinery, which Applicants confirmed by RNA-FISH.

Epithelial subsets downregulated genes involved in fatty acid metabolism (FIG. 27C), possibly due to reduced production of short chain fatty acids by the gut microbiota. Within specific subsets, chemosensory tuft cells upregulated the diamine oxidase, AOC1, which may degrade mast cell-produced histamine (FIG. 27F); goblet cells increased importers of sialic acids (FIG. 27F), which may promote the growth of Escherichia coli; cycling TA cells upregulated IL-23, a key cytokine implicated in IBD through GWAS; and goblet cells and enterocytes upregulated genes for retinoic acid (RA) biosynthesis (FIG. 27F), while M cells induced the RA binding protein, CRABP2 (FIG. 27F). RA is known to suppress intestinal mucus production and to exacerbate colitis, suggesting that M cells may play an important role in this process.

Within the stromal compartment, expression changes reflected induction of inflammatory cues, tissue repair and fibrosis, and of vascular expansion in the supporting tissue, suggesting a major role of the stroma in disease progression. Multiple subsets activate pro-fibrosis programs, including upregulation of genes involved in collagen deposition and fibrosis (FIG. 27D), expression of beta-catenin (CTNNB1; FIG. 27D), a mediator of pro-fibrotic WNT signaling by crypt-associated fibroblasts, and expression of fibrosis-associated ECM components that are normally restricted to the crypt (e.g. DCN, LUM; FIG. 27D,G) by villus-associated fibroblasts (FIG. 27D). In contrast to the dramatic increase in CAIFs, other fibroblast subsets downregulated the chemokines CCL8, CXCL12, and CCL13 (FIG. 27D,G) and produced neprilysin (MME), a metalloprotease that cleaves peptide hormones, including substance P, which could limit inflammation (FIG. 27D). Post-capillary venules induced CSF3 (FIG. 27G), which signals for the growth and differentiation of monocytes and granulocytes, and endothelial cell subsets induced angiopoietin 2 (ANGPT2; FIG. 27G) and the adhesion glycoprotein, THY1 (FIG. 27D), which may promote angiogenesis and leukocyte recruitment into the diseased tissue.

Although innate immune responses seem to be a prerequisite for the excessive activation of adaptive immunity, the latter is the more proximate driver of tissue damage in UC. In particular, multiple subsets of CD4⁺ and CD8⁺ T cells adopted a Th17-like phenotype, with upregulation of both IL-17 (IL17A, IL17F; FIG. 27E) and of checkpoint genes (e.g. CTLA4, PDCD1, TIGIT; FIG. 27E). IL-17 expressing cells promote a pro-inflammatory and cytotoxic immune response, which may be reinforced by the expression of cytotoxic granule genes (e.g. GZMK, GNLY; FIG. 27E) in all subsets of CD8⁺ T cells, and which may contribute to epithelial tissue damage. More generally, all CD8⁺ T cells induced cytotoxic programs in inflamed tissue that was accompanied by the expression of a co-inhibitory, checkpoint molecule (FIG. 28A). Notably, checkpoint activation was already apparent in healthy tissue, which may explain immunotherapy-induced colitis in some cancer patients. Within B cells, the increased expression of the TFs PAX5, IRF8, and BCL6 in multiple subsets and the expression of AICDA in GC B cells, which promotes affinity maturation and class switch recombination, help explain the reduction in plasma cells (FIG. 27A) and IgG class switching (FIG. 38). Finally, few changes were shared across the myeloid lineage, whereas subset specific changes reflected modulation of the innate immune response in monocytes (induced calprotectin, an inflammatory biomarker of UC and reduced FCER1A and MHC II), DCs (increased expression HTR3A and IL22R, suggesting increased interaction with mast cells and Th17 cells, respectively); and CD69⁺ mast cells (upregulated secretory granule genes).

Example 9—Shift in Carbon Metabolism, Fatty Acid Oxidation and Amino Acid Metabolism in Epithelial Cells in UC

Comparison of non-inflamed and inflamed tissue within UC patients revealed several metabolic changes within epithelial cells that may underlie tissue inflammation (FIG. 28E). The expression of purine metabolism genes (e.g. XDH, URAD; FIG. 27C,F) was altered in epithelial subsets, likely leading to the production of uric acid. Uric acid is induced by S. cerevisiae colonization, leading to epithelial damage in mice, and inhibition of uric acid synthesis can ameliorate colitis (e.g., damage is reversed upon inhibition of uric acid synthesis). Epithelial cells in inflamed tissue also reduce HMGCS2, the limiting rate enzyme that catalyzes the first reaction in ketosis, and increased the expression of enzymes in the kynurenine pathway, a pathway that is associated with disease severity [REF] and is thought to promote mucosal inflammation through the rewiring of tryptophan metabolism and the abrogation of IL-22 synthesis (e.g. IDO1, KYNU), which may replenish NAD+ levels for oxidative phosphorylation. Diminished CLCA1 expression by secretory TA cells in inflamed tissue may help explain defects in the mucus layer thickness during inflammation. Such rewiring of epithelial cell metabolism in inflammation in UC is consistent with studies suggesting that stress and inflammation are coupled to the upstream sensing of nutrients, such as carbohydrates, lipids, and amino acids.

Previous studies suggest that stress and inflammation pathways induced in IBD and consisting of many IBD GWAS genes may be coupled to upstream environmental sensing of nutrients, such as oxygen, fatty acids, and amino acids, which in turn may be impacted by the microbiota. To identify such metabolic changes systematically, Applicants scored changes in the expression of 239 pathways related to nutrient sensing, stress, and inflammation across all cell types (FIG. 28E), relative to a background set of genes selected to have similar expression profiles across all samples.

This analysis revealed metabolic shifts between oxidative phosphorylation and glycolysis, and changes in fatty acid and amino acid metabolism. First, in UC, epithelial cells shifted their metabolism from oxidative phosphorylation to glycolysis and the pentose phosphate pathway (FIG. 28E), while immune cells shifted towards oxidative phosphorylation, which may reflect efforts to quell immune activity, often coupled to glycolysis, which reflect efforts to quell immune activity, often coupled to glycolysis. Second, across multiple subsets Applicants infer a switch from microbial to dietary sources of fatty acids. There is reduced expression of pathways for beta-oxidation and the metabolism of butyrate and propionate (FIG. 28E), likely driven by impaired production of short chain fatty acids (SCFAs) by the gut microbiota, along with increased expression of dietary fatty acids metabolism genes (FIG. 28E) by epithelial cells in non-inflamed and inflamed tissue. Finally, epithelial cells from non-inflamed and inflamed tissue increased expression of pathways for the biosynthesis of arginine and the metabolism of alanine, aspartate, and glutamate, and reduced the metabolism of valine, leucine, isoleucine, lysine, and histidine (FIG. 28E). Changes in amino acid sensing may explain elevated levels of mTORC1 signaling across multiple subsets (FIG. 28E). Although metabolism of tryptophan through the kynurenine pathway increased, the combined gene signature for tryptophan metabolism decreased in epithelial cells and fibroblasts (FIG. 28E).

Example 10—Induction of a Strong IL17 Response and Checkpoints in CD8+ Cells in UC

Although the innate immune response seems to be a prerequisite for the excessive activation of adaptive immunity, the latter is the more proximate driver of tissue damage in UC [REF]. In particular, multiple subsets of CD4⁺ and CD8⁺ T cells adopted a Th17-like phenotype, with upregulation of IL-17 (IL17A, IL17F; FIG. 27E) and checkpoint genes (e.g. CTLA4, PDCD1, TIGIT; FIG. 27E). The CD8⁺IL-17⁺ cells promote a pro-inflammatory and cytotoxic immune response, as well as induce the expression of IL23R in non-inflamed and inflamed tissue. This may be further reinforced by the expression of cytotoxic granule genes (e.g. GZMK, GNLY; FIG. 27E) in all subsets of CD8⁺ T cells, and which may contribute to epithelial tissue damage. More generally, all CD8+ T cells induced cytotoxic programs in inflamed tissue that were accompanied by the expression of a co-inhibitory, checkpoint molecule (FIG. 28A). Notably, checkpoint activation was already apparent in healthy tissue, which may explain immunotherapy-induced colitis in some cancer patients.

Example 11—a Shift of TNF Responding Cells to CAIFs May Underlie the Resistance to Anti-TNF Therapy

The differentially expressed genes highlight inflammatory processes occurring in the different stages of colitis from non-inflamed to inflamed tissue across diverse cells. TNF signaling is one of the key pathways contributing to the onset and progression of UC, and monoclonal anti-TNF antibodies have been a major breakthrough in the treatment of IBD. Despite this success, non-response rates are high and treated patients eventually develop resistance to treatment, suggesting that there are both intrinsic and acquired causes of resistance. Additional inflammatory pathways could participate in gut inflammation as etiological causes, effects, or exacerbating factors. To assess those, Applicants compared each cell subset for the change between healthy, non-inflamed and inflamed tissue in seven inflammation signatures, as well as in expression of the TNF response (FIG. 28B,C).

The transition from healthy to non-inflamed tissue was mostly marked by induction of pathways within fibroblasts. For example, TNFα signaling increased in WNT2B+Fos^(lo) fibroblasts and myofibroblasts, Jak-STAT signaling increased in WNT2B⁺ and WNT5B⁺ subsets, and TGFβ signaling increased in myofibroblasts (FIG. 28B). Additional pathways were induced in inflamed tissues across multiple lineages, including increases in IFNα/β and IFNγ signaling in epithelial subsets, B cells and CD69⁺ mast cells, and increases in TNF signaling among some epithelial cells, CD8⁺IL-17⁺ T cells, GC B cells, and CAIFs. This suggests that TNFα, TGFβ, and Jak-STAT responses in fibroblasts are more related to disease etiology, whereas additional pathways in epithelial cells, mast cells, and B cells are secondary aspects that exacerbate tissue inflammation. This may explain why anti-TNF drugs effectively treat UC symptoms, whereas anti-IFNγ therapy does not.

Remarkably, the largest change in TNF signaling between non-inflamed and inflamed tissue was found in CAIFs (FIG. 28C), suggesting that these cells may underlie resistance to anti-TNF therapy. To test this hypothesis, Applicants scored each subset for gene signatures related to drug resistance and sensitivity, based on a meta-analysis of bulk expression profiles from 55 drug responders and 55 non-responders to anti-TNF blockade (STAR Methods). Supporting the hypothesis, the drug resistance signature was strongly enriched in CAIFs (FIG. 28D,F; e.g. IL13RA2, ILI1, and TNFRSF11B) and inflammatory monocytes (FIG. 28D,F; e.g., G0S2, OSM, TREM1), while the drug sensitivity signature was enriched in epithelial cells (FIG. 28D,E; e.g., LGR5, PYY, RETNLB). In fact, the three genes whose expression is most significantly associated with drug resistance, IL13RA2, IL11, and TNFRSF11B, are highly specific markers of CAIFs, and are not expressed by any other cell subsets. Confirming these results, deletion of IL13RA2 ameliorates colitis in mice [REF], while pre-treatment expression of OSM is predictive of anti-TNF resistance in a human clinical trial, although the specific cell subsets or pathways mediating this resistance are unknown.

Moreover, after removing overlapping genes between the gene signatures (STAR Methods), the TNFα signature score was strongly correlated to the drug resistance score (FIG. 28D, left) and mutually exclusive with the drug sensitivity score (FIG. 28D, right), suggesting a direct relationship between TNF signaling and clinical resistance. Thus, TNF signaling by these cell subsets, particularly CAIFs, may reflect disease severity or even underlie drug non-responsiveness.

Example 12—Inter-Compartmental Re-Wiring of Cell-Cell Interactions in UC Through CAIFs, Inflammatory Monocytes, and M Cells

Both cell subset proportions and intrinsic expression levels are changed in UC relative to healthy controls. Applicants hypothesized that alterations in cell subset proportions could be explained, at least in part, by cell intrinsic changes in cell-cell interaction genes, such as cytokines, chemokines, growth factors, and their cognate receptors. For example, immune signaling in inflamed tissue was impacted by changes in both stroma and immune cells compared to non-inflamed tissue. For example with multiple fibroblast subsets decreased expression of CCL13 and increased expression of the CGRP receptor (RAMP1) (FIG. 33) or T cell subsets increasing expression of the B cell chemoattractant, CXCL13 (FIG. 39C) and the checkpoint gene, PDCD1. For example, several expression changes targeted immune signaling within inflamed tissue, including the downregulation of CCL13 in fibroblast subsets (FIG. 33) and the upregulation of CXCL13 in T cell subsets (FIG. 39C), which can propagate into the infiltration, expansion, or inhibition of other cell types. Such intrinsic changes in expression in one cell type, can propagate into the infiltration, migration or expansion of another cell type, reflected in turn by a change it its proportion and/or its state. To test this hypothesis, Applicants first mapped thousands of literature-supported receptor-ligand pairs onto the cell subsets to construct a putative cell-cell network (STAR Methods) for healthy (FIG. 29A), non-inflamed (FIG. 29B), and inflamed (FIG. 29C) tissue, and identified those cell subset pairs with a statistically significant excess of receptor-ligand connections compared to a null model.

Whereas the healthy cellular network was mostly compartmentalized, with cell-cell interactions enriched among subsets from the same lineage (FIG. 29A,D), differential expression in disease preferentially targeted cross talk across compartments, and reduced compartmentalization (FIG. 29B-D), with colitis-associated subsets, such as CAIFs, inflammatory monocytes, and M cells, as key cross-compartment connectors. Intra-compartment interactions in health delineated the epithelial compartment (P<10⁻⁴; all p-values for interactions from network permutation tests, STAR Methods) and spanned many connections reflecting homeostatic tissue organization, such as between DC1s and T cells (e.g. P<10⁻³ for T_(regs), CD8+ LP, and CD4+ Activated Fos-hi T cells), glia, endothelial cells, and pericytes (possibly comprising the gut-vascular barrier; P<0.05 for all pairs), and M cells and T cells (P<0.05 for cycling and CD8+ IEL subsets) (FIG. 29A). Conversely, in both non-inflamed and inflamed UC tissue, CAIFs, M cells, and inflammatory monocytes are the nexus of multiple intracompartmental connections. Differential expression in non-inflamed UC tissue (FIG. 29B,D) significantly targeted cross-talk between epithelial cells and T cells (P<10⁻⁴) and fibroblasts (P<10⁻⁴). Interactions between enterocytes and other cell subsets were especially targeted in non-inflamed UC tissue, including with several subsets of T cells (P<0.05 for Tregs and CD8+ IELs, P<10⁻³ for MT^(hi) T cells) and fibroblasts (e.g. P<10⁻⁴ for WNT2B⁺Fos^(lo) subsets, P<10⁻³ for WNT5B⁺ subsets). Inflamed mucosal tissue (FIG. 29C,D) showed significant re-wiring of communication between B cells and T cells (P<10⁻⁴; e.g. P<0.05 for PD1⁺ T cells and all B cell subsets), macrophages and CD8⁺IL-17⁺ T cells (P<0.05), and enterocytes and post-capillary venules (P<10⁻⁴).

Example 13—Cell-Intrinsic Changes that Underlie Immune Cells Infiltration, Stromal Cell and CAIF Proliferation and Epithelial Cell Differentiation Changes in UC

Next, Applicants systematically queried all pairs of cell subsets, by testing, for each ligand-receptor pair that was differentially expressed during disease, whether the ligand's expression level in one cell type was correlated with the frequency of the cells expressing its cognate receptor across samples (including cells of the same type, to capture both autocrine and paracrine interactions).

The results strongly support the hypothesis that re-wiring of the cell-cell signaling network may drive changes in the cell subset proportions in UC. One set of interactions explains changes in immune cell proportions by effects on their migration and infiltration. For example, the increase in FO B cell proportions within the immune compartment, one of the most significant changes Applicants observed in UC (FIG. 27A), is correlated with strong upregulation of CXCL12 in WNT2B⁺Fos^(lo) fibroblasts in UC (FIG. 29D), known to recruit B cells and induce follicle formation, and whose receptor, CXCR4, is expressed on plasma cells, (FIG. 29D, Spearman's p=0.44). In another example, the expression of IL-18, an epithelial-derived cytokine induced in enterocytes within inflamed tissue, is correlated with the frequencies of T_(regs) across samples, which express its receptor IL18R1 (FIG. 29D, Spearman's p=0.68). IL18R1, inhibits colonic Th17 differentiation, is critical for T_(e)g-mediated control of intestinal inflammation, and has been associated with IBD through GWAS.

Second, within the stroma, multiple interactions reflect expansion of a stromal cell subset through growth factors expressed by other cells. For example, there is a high correlation across samples between the induction of platelet-derived growth factor (PDGFD) in WNT2B⁺TFos^(hi) fibroblasts and the frequency of pericytes, which express its receptor, PDGFRB (FIG. 29D, Spearman's p=0.59). PDGF plays an important role in blood vessel formation.

Third, some interactions reflect an impact of immune cells or fibroblasts on cell differentiation or state transition among epithelial cells, which can impact epithelial repair. For example, the frequency of enterocytes across samples was correlated with the expression by CD4⁺ Activated Fos^(hi) T cells of IL-22, a cytokine that promotes mucosal healing and epithelial renewal known to be reduced in (FIG. 29D, Spearman's p=0.55). Conversely, there is a negative correlation between CAIFs expression of CYR61 and the proportion of enterocytes, which express its receptor, ITGAV (FIG. 29D, Spearman's ρ=.−0.76). Interestingly, RBP4 expression in enterocytes is positively regulated with the proportions of CAIF, which express its receptor (FIG. 29D), suggesting a negative feedback loop between these two cell types.

Finally, autocrine signals may regulate cell frequencies both positively and negatively. For example, BEST4+ enterocytes expression of the hepatocyte growth factor-like gene, MST1, is strongly correlated to their frequencies across samples (FIG. 29D, Spearman's p=0.66), and they express its receptor, MST1R (implicated in IBD through GWAS). Similarly, post-capillary venule expression of TRAIL, for which they express the receptors, TNFSF10B, C and D, is negatively correlated to their frequencies across samples (FIG. 29D, Spearman's rho=0.38).

Applicants integrated this analysis across multiple interactions with LASSO regression, to predict the frequency of each cell subset using the expression levels of all cognate ligands of its receptors in other cells (FIG. 29E, STAR Methods). These provided highly significant explanation to the variance in the proportion of some of the key interacting cells, including inflammatory fibroblasts, CD8+IL17+ T cells, and M cells (FIG. 29E and FIG. 37). For example, the frequencies of CD8⁺IL-17⁺ T cells were explained by the combination of positive signals from (1) autocrine sources through CCL5, and FASLG; (2) CDH1 by absorptive TA cells, which may mediate adhesion between these cells and epithelial cells; (3) CCL4 by CD8⁺ IELs and (4) IL-18 by immature enterocytes, both are known T cell chemoattractants; and (5) negatively regulation by CCL13 from WNT2B⁺Fos^(lo) fibroblasts and (6) plasma phospholipid transfer protein (PLTP) from glia.

Example 14—Mapping Disease Associated Variants to Cells of Action and Putative Function

Tissue profiling of patients with active disease captures the pathological state of the tissue, but cannot directly distinguish between cause and effect. Conversely, Genome Wide Association Studies (GWAS) can identify genetic variants that are causally associated with disease risk, but cannot readily determine the molecular, cellular and physiological function of each variant. Tissue profiling by scRNA-Seq can help map variants to function at scale, by determining the cell of action for each associated gene and the genes' differential expression pattern in disease.

Mapping 117 IBD-associated GWAS genes onto the colon cell atlas showed that 53 of the genes were strongly enriched within specific cell lineages (FIG. 30A), with 40 genes significantly differentially expressed in the cells between health and UC (FIG. 30A, Table 2, Table 13). In addition to many known associations (e.g. RNF186 in epithelial cells, CARD9 in monocytes), Applicants recovered many previously unappreciated associations. For example, Omentin (ITLN1), a receptor for bacterial arabinoglycans and lactoferrin, is expressed specifically by immature goblet cells that decreased in frequency with disease (FIG. 27A), rather than by all goblet cells; and plasma B cells expressed high levels of the NOD-like receptor, NLRP7, which is thought to recognize microbial acylated lipoproteins and activate the NLRP7 inflammasome in macrophages.

Some cell types are particularly enriched for UC-induced GWAS genes, most notably M cells, CD8⁺IL-17⁺ T cells, GC B cells, enterocytes, DC2s, and ILCs (FIG. 30B). In particular, multiple IBD-associated GWAS genes were significantly higher in M cells than in all other cell subsets, including MST1R, the receptor for macrophage-stimulating protein, CCL20, NR5A2, NFKB1, and JAK2 (FIG. 30A,B), and those geens were induced in M cells in UC vs. healthy tissue (FIG. 30B). Other cells with high mean expression levels of GWAS genes include many UC-related cell subsets, such as CD8⁺IL-17⁺ T cells, GC B cells, enterocytes, DC2s, and ILCs (FIG. 30B,C). Taken together with the changes in M cell proportions, their central cross-compartment interactions and overall differential expression patterns, this suggests that M cell dysfunction may play an underappreciated but pivotal role in UC.

Next, Applicants hypothesized that the variation in expression across individual cells of the same subset can power us to predict the function of GWAS genes. Past approaches to infer function from expression data often use “guilt by association” across bulk tissue samples, but those cannot distinguish between expression and cell proportions changes. In contrast, Applicants can measure the co-variation of genes across single cells within one cell subset, allowing us to isolate co-regulated biological processes (STAR Methods).

Using this approach, Applicants annotated many GWAS genes with new putative biological functions. For example, the function of Clorf106, expressed specifically by epithelial cells, was unknown until Applicants recently showed it was involved in cell-cell junctions. The gene module for this gene within epithelial cells contains many other genes involved in cell adhesion, including E-cadherin (CDH1), tight junction protein 3 (TJP3), and LAMB3, and is significantly enriched for the GO term “cell adhesion” (q-value <10⁻³, Fisher exact test), second only to the response to interferon-gamma, which may reflect a relevant physiological pathway. NLRP7 is a NOD-like receptor that has been shown in macrophages to trigger the assembly of the inflammasome, activation of caspase 1, maturation of IL-1B and IL-18, and rapid pyroptosis. However, the analysis suggests that within plasma B cells, NLRP7 may activate caspase 3, the highest scoring gene in the module. Other top genes include pro- and anti-apoptotic factors, including death-associated protein (DAP), Fas apoptotic inhibitory molecule (FAIM), and BIM (BCL2L11), a key regulator of BCR-mediated apoptosis. Inflammasome assembly can lead to the activation of caspase 3 in cells that do not express caspase 1, which may explain the differential responses observed in macrophages and B cells.

RNF186 is an E3 ubiquitin ligase that is thought to participate in ER stress-mediated apoptosis and is expressed uniquely in epithelial cells (FIG. 30A).

Example 15—GWAS Genes are Explained by a Small Number of Modules Spanning Key Pathways and Cells

Remarkably, in many cases, multiple IBD-associated GWAS genes map into each others' modules, allowing us to arrange 10 meta-modules that together span nearly 50% of all IBD genetic associations, and may reflect some of the key pathways in the disease (FIG. 30C). In particular, the PTPN22 module in UC Tregs contains 8 IBD-linked genes, including PTPN22, IL23R, RORC, CCL20, ATG16L1, SKAP2, PRDM1, and RASGRP1 (ranks 1, 2, 5, 17, 39, 40, 50, and 98 out of 16,801 analyzed genes, respectively). PTPN22, IL23R, RORC, and ATG16L1 are among the strongest risk factors of IBD, yet their precise roles in the disease are unknown. However, this module also contains caspase-8, BIM, and several other genes enriched in the KEGG terms for apoptosis and TNF signaling (q-value <10⁻⁴ for both terms, Fisher's exact test), suggesting that it may reflect pathways that regulate T_(eg) apoptosis vs. survival in response to TNF. In another example, the TNFAIP3 module in healthy DC2s contains 7 IBD-linked genes, including TNFAIP3, TNFSF15, PLAU, STAT4, AHR, NDFIP1, and NCF4 (ranks 1, 11, 12, 21, 25, 88, and 96 out of 15,685 analyzed genes, respectively). This module was significantly enriched for KEGG terms related to TNF and NFKB signaling (q-value <10⁻⁴ for both terms, Fisher's exact test), along with the expression of several pro-inflammatory and anti-inflammatory cytokines and their receptors (e.g. IL-8, CXCR3, IL-10, IFNGR2, IL10RB), suggesting that this module may regulate DC responses in healthy tissue. In many cases, the genes in these modules are most highly expressed in other cell types, suggesting that the co-regulation of genes within single cells, rather than their absolute levels of expression, may reveal the cell-of-action for at least some GWAS-implicated genes. Some gene modules, such as the TNFAIP3 module in DC2s, were only found in healthy cells and may thus contribute to IBD onset, but the majority of gene modules, such as the PTPN22 module in T_(regs), were only found in UC cells and may thus contribute to IBD progression (FIG. 30D). Notably, while, GWAS-enriched gene modules were found in subsets of epithelial cells, microvascular cells, myeloid cells, T cells, and B cells, but not fibroblasts, other endothelial cells, or glia (FIG. 30D), suggesting that stromal cells may contribute less to the overall genetic disease risk.

Example 16—Co-Regulation of Genes within Single Cells, Rather than their Absolute Expression Levels, Helps Recovers Causal Genes from Candidate Regions of Genetic Association

Finally, Applicants hypothesized that cell type specific expression and co-expression modules can help pinpoint the specific genes that underlie the signal of association for each IBD-related SNP haplotype. To this end, Applicants retrieved all genes associated with each original associated region variant, and for each such candidate gene set, then examined whether the gene's expression level, degree of differential expression, or co-regulation with other candidate genes could be used to successfully recover the “causal” IBD-associated gene, as defined separately by fine mapping (STAR Methods), relative to a null model in which genes were randomly selected. In the null model, the “causal” IBD gene was selected 18 out of 53 total times from gene sets ranging in size from 2-10 genes (mean=4 genes). However, using scRNA-Seq data, Applicants successfully recovered 24 “causal” genes by selecting genes with the highest gene expression from each set of candidate genes (i.e. 33% increase in accuracy), and recovered 28 “causal” genes by selecting genes that were found in the largest co-regulated gene modules consisting of other candidate genes (i.e. 56% increase in accuracy). Importantly, the latter method constructs modules using only candidate genes as seeds, and thus does not rely on any a priori knowledge of disease associations, aside from the genetic regions and the scRNA-seq data. Furthermore, scRNA-seq data can also help prune candidate gene sets to reduce the number of potential hits, by removing genes with no detectable expression in the colon cells, genes that were not differentially expressed, or genes that were not found in any gene modules of candidate genes. Filtering by expression, Applicants successfully eliminated 18 out of 139 total genes, while incorrectly eliminating 5 true hits. Using modules, Applicants successfully eliminated 45 of 139 total genes, while incorrectly eliminating 9 true hits. Taken together, these results suggest that the co-regulation of genes within single cells, rather than their absolute levels of expression, can help recover the causal genes from candidate gene sets. Combining both ranking by co-expression and filtering, Applicants inferred the IBD-associated genes for all regions where the underlying variant is not known (FIG. 30E). This analysis suggests roles for NCF4, PDGFB, IL10, and CCRL2 in IBD.

Example 17—Discussion

The single cell census of the healthy and IBD colon generated a comprehensive cellular and molecular map of health and disease. This revealed nearly all known cell types, with the notable exception of neutrophils, revealed new cell types and states in the colon, including a subset of chemosensory epithelial cells that may detect pH and contribute to sour taste perception in the colon. Comparison of the cellular composition between healthy, uninflamed and inflamed UC tissue highlighted key disease-specific cell subsets whose contributions to IBD were largely unknown. Analysis of cell intrinsic programs showed that transcriptional programs are larger similarly changed in non-inflamed and inflamed tissue compared to healthy tissue, suggested that non-UC tissue, albeit histologically seemingly normal, is substantially modified, either as a “pre-inflamed” state or as “post-resolution”. Analysis of cell interactions showed substantial rewiring from healthy to uninflamed to inflamed, with increased cross-talk between compartments, and allowed to explain some of the most dramatic changes in cellular proportions through cell-cell interactions that impact cell infiltration, proliferation and differentiation. The magnitudes of these reported changes—in cell proportions, intrinsic programs, and cell-cell interactions, emphasize the layer of complexity of colitis in which the three major components of the colon; the epithelial, stromal and immune cell are able to contribute to the initiation and progression of the disease, both inherently and through their effects on each other.

Several cell types, including M cells, CAIFs, inflammatory monocytes, B cells, and CD8⁺IL-17⁺ T cells—stand out as particularly prominent in disease and are often the locus of expression of GWAS genes—and manifest both changes in proportions, expression programs, and cell-cell interactions, that can play a role in disease initiation, progression and drug resistance, thus substantially revising the cellular and molecular narrative of disease.

BEST4+ Enterocytes are a New Subset of Chemosensory Epithelial Cells

Within the colon, pH sensing and sour taste perception may help detect members of the gut microbiota, for example, the lactic acid bacteria, many of which have established long-term symbioses with the human host and are thought to inhabit colonic crypts. Recent studies have highlighted the role of tuft cells in chemosensation at the microbiota-epithelium interface. The atlas uncovered also BEST4+ enterocytes, a new subset of chemosensory epithelial cells, which Applicants validated in the colons of healthy subjects and IBD patients (FIG. 26B). These cells may help detect and modulate salts and acids, and may work alongside tuft cells to transduce taste signals in the intestine. Supporting this hypothesis, they share the TF, SPIB, with tuft cells and M cells, suggesting either a developmental link or a common regulon for their shared functions. That this cell type has not been observed in the earlier census of the mouse small intestine may relate to either species-specific differences or to pH differences between the small and large intestines. Alternatively, as regulators of salt balance, these cells could be involved in water absorption, a key function of the colon, but not the small intestine. This interpretation is supported by low expression of renin in these cells. The proportion of BEST4⁺ enterocytes, along with those of several other epithelial subsets, are modestly decreases in inflamed tissue (FIG. 27A) and few differentially expressed genes with disease. Applicants found significant autocrine and paracrine signals controlling their abundances; most notably, their expression levels of MST1, for which they express the receptor, MST1R, were strongly correlated to their proportions across samples (FIG. 29D).

Microfold Cells are Expanded in Disease, Mediate Epithelial-T Cell Interactions, Especially with T_(regs), and are Enriched for GWAS Genes

Microfold cells are critical for the recognition of the gut microbiota by the adaptive immune system and were previously reported to reside in GALT (e.g. isolated lymphoid follicles) in healthy subjects. Microfold cells were rarely detected in healthy subjects, but expanded substantially in multiple inflamed tissue samples (FIG. 27A), which was unexpected because most biopsy specimens do not capture GALT (e.g. isolated lymphoid follicles). Their expansion during disease may either reflect the development of tertiary lymphoid structures or expansion of small sentinel populations of M cells within normal epithelium, and suggests that they may play an important and previously unrecognized role in the disease. In the cell-cell network, M cells are the sole epithelial cell type in the T cell compartment in healthy tissue, and are a central hub leading to the increased cross-compartment connectivity in non-inflamed and inflamed tissue, especially through connections to myeloid cells (FIG. 29A-C). Notably, within inflamed tissue, as epithelial cells overall increase production of RA, M cells upregulate the RA binding protein, CRABP2. RA production by DCs leads to the development of gut-homing T_(regs) and it is possible that RA sequestration by CRABP2 from M cells plays a similar role, which also present antigen and form intimate associations with T cells. Moreover, M cells were major producers of CCL20, a cytokine whose expression in enterocytes and M cells was correlated in the analysis to the frequency of T_(regs) across samples (FIG. 29D). Finally, the analysis implicates M cells causally in IBD through their expression of “GWAS genes”: Indeed, they have the highest mean expression of all IBD-associated GWAS genes (FIG. 30A), including the highest expression levels of CCL20, JAK2, NFKB1, and NR5A2 (FIG. 30A), and an M-cell expressed gene module consist of 5 IBD-associated, co-regulated GWAS genes, including CCL20, ERAP1, PTGER4, JAK2, and TMEM135.

Inflammatory Fibroblasts and Inflammatory Monocytes are Key Hubs and May be Associated with Response and Resistance to Anti-TNF Therapy

CAIFs are a new subset of fibroblasts that were barely detectable in healthy tissue, increased in non-inflamed tissue from UC patients, and dramatically expanded in inflamed tissue from UC patients (FIG. 27A). Together with inflammatory monocytes, the two cell types were strongly associated with signatures of clinical resistance to TNF blockade (FIG. 28D). This association may arise either because these cells are biomarkers of disease severity or are actively involved in drug resistance. Supporting the latter possibility, CAIFs uniquely express several genes that may promote resistance, including IL13RA2 and IL11, while inflammatory monocytes highly express OSM and ILIRN. Both subsets also express high levels of IL-8 and kynurenase (KYNU), which is a known biomarker of disease severity. Applicants additionally found: CAIFs interact with enterocytes; CAIFs and monocytes are “hubs” in disease interaction networks; and Few GWAS genes map to CAIFs.

T Cells

Applicants uncover strong evidence for the role of CD8⁺IL-17⁺ T cells and Tregs in in IBD, which both progressively increase in frequency from healthy to non-inflamed to inflamed tissue (FIG. 27A). CD8⁺IL-17⁺ T cells were previously found in UC patients, but their role in the disease was unclear and they were not known to comprise a large fraction of colon-resident T cells. Surprisingly, these and other T cells simultaneously induce cytotoxic and co-inhibitory pathways. Applicants additionally found: Tregs upregulate TNF with disease; CD8 cells interactions (autocrine+paracrine interactions); and Re-wiring of T cell interactions with disease; GWAS modules show that Tregs and CD8 T cells are important (apoptosis).

This analysis provides a framework for using scRNA-Seq to understand complex diseases, from a census of cell types and states within healthy and diseased tissue, to identifying changes in cell proportions with disease, and partitioning changes in gene expression into those that are shared by cell lineages or unique to cell subsets or to drug responses; then, integrating these analyses to understand how changes in gene expression propagate into changes in cell-cell interactions, identifying the “cell-of-action” for GWAS genes, and understanding the complex genetic risk factors for the disease.

TABLE 3 Epithelial Healthy specific markers for indicated cell types E.Enterocyte_Immature_1 SLC16A12, TAC1, EFCAB5 E.Enterocyte_Immature_2 RP11-525K10.3, RP11-576122.2, DRD5, LINC00974, GDPD2 E.Enterocyte_Progenitor, RP11-800A18.4 E.Enterocytes KIAA1239, RP11-396O20.1, DUSP21, SLC7A9, ARTN, SAA1, RP11-266L9.5, RP11-77K12.7, RBP2, SLC14A2, ADAMTSL4-AS1, RNU6-1016P, HAS3, LINC00955, G6PC, SAA2, CTB-58E17.9, KCTD4, SLC22A1, CELA3A, SLC6A20, CELA3B, CTC-490G23.2, CTB-171A8.1, GPR110, MAB21L3, RP11-30P6.6, SLC45A2, RAB6B, RP11-202A13.1, RP11-116O18.1, EMP1 E.Enteroendocrine DNAH2, MNX1, TNNC1, DACT2, FBXL16, RAB26, RP11-17M24.1, CNNM3, RP11-279F6.1, SYT13, AC114730.3, ADPRHL1, KIAA1456, DDC, C19orf77, SNORD3D, SEZ6L2, STX1A, NAGS, KIF12, C14orf93, ZNF311, PTPRD, MEX3A, PPL, COLCA1, CYP4F3, HOXB9 E.Epithelial PRSS8, VIL1, PRR15L, PPP1R1B, AQP8, CCL15, SLC26A3, PCK1, CKMT1B, PRAP1, CKMTIA, LYPD8, PKP3, AKR1B10, AP1M2, PLA2G10, NXPE4, MYO1A, TMEM171, PRR15, USH1C, MS4A12, PDZK1IP1, KLK1, GGT6, FUT3, TMPRSS2, CBLC, MUC2, GUCA2B, LAD1, CDH1, MUC1, GJB1, C1orG10, LINC00035, DSG2, LINC00483, C1orf106, GPRC5A, MUC4, LAMB3, ITLN1, CLRN3, CLCA4, LINC00675, MEP1A, CYP3A5, AGR3, TRIM31, MARVELD3, ERN2, CES3, PLA2G2A, MUC5B, RP11-519G16.5, SATB2, CLCA1, MAL2, CGN, NEU4, CFTR, RAPGEFL1, FERMT1, BAIAP2L2, DDC, HNF4A, PLEKHG6, BTNL3, ARL14, CDHR2, FABP2, LCN2, SLC17A4, TM4SF5, ENTPD8, SPINK4, POF1B, MYO5B, C9orf152, VIPR1, PDZD3, COL17A1, LAMA1, PLS1, IHH, B3GNT3, TMIGD1, OVOL1, REP15, RP11-395B7.2, RETNLB, CDKN2B- AS1, GSTA1, MOGAT2, A1CF, SEMA4G, UGT2A3, BTNL8, SGK2, CEACAM6, SLC51A, YBX2, HHLA2, TFF1, TRIM15, NOX1, C11orf86, OLFM4, LRRC19, PITX2, C1orf172, RNF43, PPP1R14C, U47924.27, LIPH, CWH43, EDN3, ANXA13, CAMSAP3, PI3, TMEM184A, F2RL1, CAPN8, SMIM6, HEPACAM2, SH3RF2, TMEM82, ISX, ANKS4B, RBBP8NL, GRB7, SPDEF, ESRP1, EPB41L4B, SLC3A1, AC106876.2, LINC00668, HNF1B, RP11-747D18.1, NGEF, RP11-465B22.8, EPHA10, MB, ZBTB7C, STX19, CA7, SATB2-AS1, ASPG, RP11-680F8.1, PRAC1, NXPE2, REG1A, C12orf36, RP11-465N4.4, CTD-2626G11.2, RP11-708H21.4, SLC9A2, S100P, RP1-278O22.1, L1TD1, KIF12, INPP5J, OVOL2, AC005355.2, WNK4, NR1I2, NAT2, SMIM2-AS1, LINC00992, EDN2, BARX2, C1orf116, HNF1A-AS1, RAP1GAP, SCGB2A1, BEST2, TINAG, GPRIN2, B4GALNT2, RP11-234B24.2, TMEM236, FOXD2, RP11-349K16.1, RHOV, IL22RA1, DMBT1, RP11-304L19.1, RP11-627G23.1, SLC5A1, BEST4, XDH, AC066593.1, RASEF, GLOD5, TMED6, CELA3B, OTOP2, CAPN13, GOLT1A, TMEM61, RP11-59E19.1, GDPD2, ADH6, CYP2B6, IYD, HNF4G, CAPN9, FOXA1, WWC1, SLC30A10, SERPINA6, RP5-881L22.5, IGSF3, PLA2G4F, SLC6A7, FOXA2, MIR194-2, RP3-523K23.2, TMEM92, NOS2, RP11-30P6.6, C3orf83, SLC13A2, SYT13, AGXT, CELA3A, CTD- 2547H18.1, CTSE, EPPK1, MYRF, RBP2, TMEM72, FAM83E, GPR39, LINC00704, ACE2, FIBCD1, HOXA13, RP11-297L17.2, RP11-284F21.10, SH2D6, AC009133.21, CTD-2196E14.5, GALNT5, MEP1B, MT3, UGT2B7, CYP2C18, TUBAL3, APOBEC1, CLDN8, RP11-408H20.1, USP43, CTC-210G5.1, HAS3, CTD-2566J3.1, AC011298.2, GLRA4, HSD3B2, CTD-2047H16.2, FAM83B, HOXB13, KRT14, LINC00261, PRAC2, SLC6A19, CASC9, MUC3A, RP11-328M4.2, TM4SF20, PRLR, C6orf141, RP11-150O12.3, RP11-187E13.1, MSLN, ALPI, SI, SOWAHA, GJB3, TBX10, CHAD, RP11-191G24.1, C1QTNF1-AS1, KLK15, PYY, MRAP2, ALDOB, CYP4F2, RP11-91K11.2, RP11-567C2.1, AP000344.3, CASC8, CYP3A4, FAM151A, GRHL2, SLC1A7, TTPA, LCN12, AC007182.6, KLK3, PF4, PVRL4, RP11-542M13.2, TREH, CYP4F11, AC011523.2, GPR115, RP11-1260E13.2, RP11-519G16.3, RP11-6N17.6, MESP2, DMRTA1, AC005152.2, BRINP3, CTA- 363E6.2, GPD1, MUC17, NOVA1-AS1, OTOP3, RP11-470P21.2, RP11-595B24.2, RP11-800A3.4, TRPM5, WFIKKN1, BCMO1, GPR128, RP1-170O19.14, RP11-801F7.1, AC005550.3, ACSM1, DPP10, GPR143, HMGA2, KCNE2, LRRC66, PCSK9, PSCA, RP11-202A13.1, RP13-616I3.1, AP001610.9, DACT2, FAM160A1, HTR3E, OGDHL, RP11-28H5.2, RP11-627G18.4, RP11-64K12.10, RP11-800A18.4, SLC5A11, TRIM10, XXyac-YM21GA2.4, B3GALT1, LGR5, RP11-223110.1, RP11-290F24.6, RP11-379B18.6, RP11-93B14.5, RXFP4, UGT1A10, CHGA, DNAH3, C19orf45, CTD-3010D24.3, GNG13, KRT12, LINC00520, NR0B2, RP11- 116O18.1, RP11-135A1.2, RP11-276H7.3, RP11-509E16.1, SHH, TFF2, TNNT2, UCA1, RP11-125B21.2, ABHD12B, CTA-221G9.11, CTC-55802.1, DAO, GPR98, LGR6, RP11-432J24.2, RP11-644F5.10, RP4- 680D5.8, RP5-1057J7.7, SLC15A1, SLC9A3, TAC1, TRPC7-AS1, LHX4, CASC16, CCDC108, CHRM3, CTD- 2611O12.7, KCNK10, KNG1, LINC01071, OXGR1, PHYHIP, POU2F3, RP11-1069G10.1, RP11-1220K2.2, RP11-188P20.3, RP11-339B21.15, RP11-695J4.2, RP11-771K4.1, RP11-809C18.4, SLC45A2, XX-CR54.3, AC024592.9, AC083900.1, AC090673.1, CTD-2026G6.3, CTD-2589M5.4, DUOXA2, GALNT8, HSD17B3, INSL5, KCNV1, KLHL34, LA16c-395F10.2, LINC00941, MAB21L3, RP11-227H15.4, RP11-416N2.4, SLC5A10, SYTL5, FRRS1, AC064834.1, AQP12A, C12orf56, C1orf177, C4BPA, CHST5, CTB-25B13.6, DEFA5, DLG3-AS1, FAM83H-AS1, FEV, GLTPD2, HIST1H4B, LINC00114, LINC00570, MT-TS2, POU5F1B, PRDM7, RP11-209E8.1, RP11-320N21.2, RP11-392E22.12, RP11-426L16.3, RP11-74C1.4, RP11-757F18.5, RP11-806O11.1, RP11-844P9.2, SLC38A4 E.Goblet CTD-2231E14.4, PLA2G2F, TFF1, TBX10, AC093642.3, RP11-95M15.1, FER1L6, S100P, LINC01022, RN7SKP127, SYTL5, FFAR4, MUC2, SBF2-AS1, RASEF, MUC1, TFF2, NRAP, GALNT5, RP11-379B8.1, HIST1H4A, LINC00842, RP11-363E7.4, AC011718.2, GPR153, RP11-845C23.2, CHAD, CHRNA7, CLDN8, GPRIN2, AC009133.21, FAM101A, SYTL2, RP11-757F18.5, BCAS1, AN RD36C, ZG16, CAPN8, SMIM6, HIST1H2BG, AN RD18A, TM4SF5, RNF39, GLTPD2, LRRC31, EIF2AK3, RECQL5, RP11-276H7.3, RP11- 196G18.22, AC147651.3, USP54, LGALS9B, DHX32, CTD-2589M5.4, TSNARE1, CYorf17, NEDD4L, HIST2H2BE, ENTPD8, SCNNIA, GALE, LINC00543, RP11-92K15.3, FAM177B, KAZALD1, HIST1H2BC, LGALS9C, FCGBP, HIST1H3D E.Immature_Enterocytes CA1, RP11-439E19.9, XXyac-YM21GA2.7, SLC26A2 E.Immature_Goblet TMEM210, ITLN1, CLCA1, LA16c-321D4.2, SPINK4, KLK15, LRRC26, KLK1, RP11-234B24.2, RETNLB, WFDC2, GNE, CCDC60, AC011523.2, LA16c-395F10.2, UGT2B7, RAP1GAP, ST6GALNAC1, AGR2, CTD- 2547H18.1, KLK3, LINC00261, CACNA2D2, GALNT8, KLK4, GMDS, TMEM61, SPINK1, PFKFB4 E.Secretory ABCC8, CTD-2231E14.4, HTR3C, NKX2-2, PAX6, PLA2G2F, PRAME, RP11-69G7.1, VWA5B2, HTR3E, GNG13, SCGN, SST, GCG, SH2D6, CHGA, TPH1, FEV, PYY, CRYBA2, SH2D7, TRPM5, TNNI1, OGDHL, POU2F3, NCMAP, TAS1R3, KLHDC7A, TFF1, TBX10, HMX2, AZGP1, TREH, AC093642.3, IL17RB, AC053503.4, FER1L6, KLK11, KCNQ4, PRSS22, SCG5, S100P, AVIL, PROC, RP11-93B14.5, LINC01022, C11orf53, SYTL5, ARHGEF38, TGM3, FFAR4, SHB, LCN15, ARX, MUC2, SBF2-AS1, BMX, RASEF, MUC1, TFF2, NRAP, ATP2A3, RP11-384L8.1, GPR153, PSTPIP2, RP11-700H6.1, TMEM198, HIST1H4A, GALNT5, PART1, RP11-379B8.1, 7SK, RP11-845C23.2, RP5-821D11.7, CTA-221G9.11, IGSF21, TM4SF5, LINC00842, RP11-363E7.4, SYT7, CHGB, AC011718.2, CHAD, GPRIN2, RP11-122G18.5, HCG9, MYCBPAP, CNTD1, CHRNA7, FAM101A, CLDN8, GFI1B, RECQL5, ANKRD36C, SYTL2, RP11-757F18.5, CTD-3051D23.4, AC009133.21, GRASP, BCAS1, ANKRD18A, SMIM6, RP11-498E2.9, RAB3B, FAM106A, CAPN8, MYRF, ARHGEF11, FUT6, ZG16, HIST1H2BG, MYO5C, ESPL1, PRUNE2, HCK E.Secretory_All HTR3C, GCG, HTR3E, GNG13, SH2D6, FEV, CHGA, SCGN, CRYBA2, ZG16, TBX10, SH2D7, TRPM5, MUC2, PYY, OGDHL, BEST2, LA16c-321D4.2, AC009133.21, CAPN9, REP15, KCNQ4, POU2F3, AC011523.2, NCMAP, MB, FCGBP, SCGB2A1, SYTL5, FFAR4, KLK12, ITLN1, CLCA1, TFF3, TAS1R3, REG4, HMX2, TMEM61, TFF1, SPINK4, FER1L6, TPSG1, RP11-234B24.2, RETNLB, KLK15, RP11-384L8.1, ANXA13, ANO7, CCDC60, HOXA-AS3, KLK1, KLK3, AC093642.3, AZGP1, LRRC26, SPDEF, IL17RB, TREH, CTD-2589M5.4, CCDC108, RAP1GAP, WFDC2, LINC00238, LA16c-395F10.2, FOXA3, LINC00261, RXFP4, CTA-221G9.11, CA9, PFKFB4, CREB3L1, S100P, GPR153, C11orf53, ST6GALNAC1, PROC, FOXP4, ARHGEF38, RP11-93B14.5, WNK4 E.Secretory_TA RP11-350J20.12 E.Stem LEFTY1, ASCL2, RGMB, CDCA7, ALDH1B1, EPHB3, OLFM4, SMOC2, PTPRO, SLC39A2, LGR5, CELF5, OXGR1, RP11-84C10.4, FAM201A, TERT, RP11-43505.2, RP11-219E7.4, FMN2, DEC1, TMPRSS13, CLDN1, SNTN, RP11-396C23.2, TRIM74, RP11-22L13.1

TABLE 4 Epithelial UC specific markers for indicated cell types E.Enterocyte_Progenitor SLC38A4, AC013268.5, AGMO E.Enterocytes BEAN1, CYP24A1, KLK8, MYZAP, PLA2G4E, PNCK, RP11-103J17.2, RP11-317L10.1, RP11-626P14.2, SERPINB4, SLC47A2, ANXA10, INSL4, SERPINB7, RP11-79H23.3, MMP7, FOXE3, SAA4, RP11-381O7.3, KIAA1239, MGAM, C8G, AC104135.3, FAM83A, GLRA4, TPRXL, RP11-30P6.6, PHYHIP, RP11-73G16.1, RP11-345J4.3, RP11-28H5.2, SLC6A14, LINC00955, RP5-1086K13.1, RAB6B, TCHP, PDZK1IP1, RP11- 35P15.1, AQP11, LINC00479, CRABP1, LY6D, BMP3, KCNG1, RP11-542M13.2, ABTB2, SLC6A20, TM4SF20, PLIN1 E.Enteroendocrine MIR7-3HG, NTS, PAX4, PAX6, VWA5B2, PYY, INSL5, SCGN, GCG, FEV, CHGA, CRYBA2, PRPH, SST, TPH1, SCG3, LCN15, KCNH6, KCNJ6, EYS, INSM1, SCG2, CPB1, RFX6, CHGB, NKX2-2, NEUROD1, CNIH2, SLC18A1, LINC00470, SCG5, NEUROG3, PCSK1N, TGM3, MEGT1, MAFA, TNNC1, PCSK1, RTBDN, CACNA1A, RP13-131K19.6, AC034243.1, SYT13, MS4A8, PDX1, ARX, SLC29A4, MAPK8IP2, STX1A, LRRC24, SCT, CTD-3193013.9, MLXIPL, BAIAP3, RIMS2, RIMBP2, DDC, C6orf141, MANEAL, AMBP, CAMK2B, CYP2W1, RXFP4, PELI3, ASCL1, RUNDC3A, PNPO, ATP6V1C2, ACVR2B, NPW, LY6H, PSCA, PPL, CADPS, PAPPA2, DUSP26, NT5DC3, RP11-279F6.1, CXXC4, DNAJC12, NOP9, Z83851.1, CELF4, PEMT, RAB26, GIPR, PGAM2 E.Epithelial ABCA12, ABO, AC005152.2, AC005550.3, AC007182.6, AC007255.8, AC007292.6, AC009133.21, AC010745.1, AC011298.2, AC011523.2, AC011718.2, AC011747.7, AC024592.9, AC026471.6, AC053503.4, AC066593.1, AC069277.2, AC090673.1, AC104667.3, AC106876.2, AC110619.2, ACE2, AGXT, AL133373.1, ALDH1A2, ALOX12B, AMBP, ANKRD18A, ANKS4B, ANO5, AP001610.9, AQP5, ARTN, B3GALT1, B4GALNT2, BCMO1, BEST2, C12orf56, C1QTNF1-AS1, C1orf168, C21orf88, C2orf54, C2orf70, C3orf83, C4BPA, C5orf52, CALN1, CASC16, CASC9, CASP16, CCDC108, CCDC60, CELA3A, CELF5, CHAD, CHRNA7, CHST5, CNTN3, COL2A1, CRABP1, CRYBA2, CRYBB3, CTA-363E6.2, CTB-175P5.4, CTC- 210G5.1, CTC-436P18.3, CTC-490G23.2, CTC-558O2.1, CTD-2377D24.6, CTD-2547H18.1, CTD-2566J3.1, CTD-2589M5.4, CTD-3010D24.3, CTD-3118D7.1, CWH43, CYP2B6, CYP2C18, CYP3A4, CYP4F11, CYP4F2, CYorf17, DACT2, DAO, DEFB4A, DMRTA1, DNAJC6, DPP10, EDN2, EGF, ENKUR, FAM151A, FAM160A1, FAM83A, FAM83B, FAM83H-AS1, FEV, FOXH1, FOXN1, FRMD5, GABRB2, GABRB3, GABRP, GAL3ST1, GALNT8, GJB4, GJB5, GLRA2, GLRA4, GNG13, GPD1, GPR110, GPR115, GPR128, GPR37L1, HMGA2, HS3ST6, HSD3B2, HSPB3, HTR3E, HTR4, IGFALS, IL37, IRX2, ISX, KCNE2, KCNK10, KIAA0319, KLHDC7A, KLK12, KLK15, KLK3, KLK4, KNG1, KRT12, KRT13, KRT14, KRT6B, KRTAP13-2, LA16c- 395F10.2, LECT1, LGR5, LHX4, LINC00114, LINC00238, LINC00639, LINC00842, LINC00896, LINC00940, LL22NC03-32F9.1, LRRC66, LRRIQ4, LYPD6, MAB21L3, MAMDC2-AS1, MEP1B, MESP2, MIR194-2, MNX1, MNX1-AS2, MT-TY, MT3, NAT2, NAT8, NKX2-2, NOVA1-AS1, NPSR1, NR0B2, NR1I2, NRAP, OGDHL, PCAT7, PLA2G12B, PLA2G4F, PLCH1, PLSCR2, RBP2, RNF183, RNU1-134P, RP1-170O19.21, RP1-240K6.3, RP1-60O19.1, RP11-1069G10.1, RP11-1157N2_B.2, RP11-11N5.3, RP11-120K24.3, RP11- 1220K2.2, RP11-150O12.3, RP11-150O12.6, RP11-164P12.4, RP11-187E13.1, RP11-188P20.3, RP11-202A13.1, RP11-206L10.3, RP11-209E8.1, RP11-211G23.2, RP11-21L23.2, RP11-223I10.1, RP11-231E6.1, RP11- 244F12.3, RP11-275F13.1, RP11-307C12.11, RP11-30P6.6, RP11-349K16.1, RP11-352G9.1, RP11-35P15.1, RP11-380P13.1, RP11-382B18.4, RP11-41O4.1, RP11-432J24.2, RP11-439E19.7, RP11-440I14.3, RP11- 44F14.8, RP11-465N4.5, RP11-469H8.6, RP11-470P21.2, RP11-511I2.2, RP11-519G16.3, RP11-542M13.2, RP11-595B24.2, RP11-627G18.4, RP11-627G23.1, RP11-63P12.7, RP11-64K12.10, RP11-680F8.1, RP11- 6N17.6, RP11-708H21.4, RP11-747D18.1, RP11-757F18.5, RP11-77K12.7, RP11-789C1.1, RP11-796E10.1, RP11-798K3.2, RP11-800A18.4, RP11-801F7.1, RP11-844P9.2, RP11-84C10.4, RP11-93B14.5, RP11-963H4.3, RP13-497K6.1, RP13-616I3.1, RP4-680D5.8, RP5-1013A22.5, RP5-1057J7.7, S100A7, SAA4, SCEL, SCGB2A1, SCGN, SEMA3B-AS1, SERPINA6, SHH, SLC10A5, SLC13A2, SLC15A1, SLC18A1, SLC1A7, SLC28A3, SLC30A10, SLC38A4, SLC39A2, SLC5A11, SLC6A19, SLC6A7, ST6GAL2, SYT8, SYTL5, TMEM72, TNNT2, TRIM10, TRIM40, TRPC7-AS1, TRPM5, TSPO2, TTC6, TTPA, TUBAL3, U47924.27, UCA1, UGT1A1, UGT2B15, UGT2B7, VSTM5, WFIKKN1, WNT11, XX-CR54.3, YBX2, SH2D6, A1CF, TMEM61, TREH, C12orf36, UGT2A3, RP11-465B22.8, NXPE2, TMIGD1, ESRP1, TBX10, FAM83E, TFF2, CDHR2, SI, GRHL2, ZG16, TMEM82, PDZD3, TM4SF5, STX19, TFF1, RETNLB, POU2F3, CELA3B, GUCA2B, RP11-234B24.2, PRAP1, C4orf19, LRRC19, APOBEC1, TRIM31, FCGBP, GUCA2A, TFF3, MUC2, GOLT1A, PCK1, LINC00992, SHD, IL22RA1, CKMT1B, MYH14, PHGR1, CDH1, HSD17B3, CEACAM5, ERN2, KBTBD12, FABP2, LAMA1, ASPG, EPB41L4B, LYPD8, SLC26A3, FERMT1, SLC17A4, CA7, HHLA2, MISP, C9orf152, ELF3, MUC13, TTLL6, TSPAN1, OVOL2, LRRC26, PPP1R14D, REP15, MSLN, C11orf86, PITX2, S100A14, AGR3, CBLC, CDHR5, CAPN8, SMIM22, KRT8, GPT, MEP1A, LCN2, LINC00675, GPRIN2, MS4A12, EPPK1, HOXB13, GCNT3, GDPD2, NXPE4, IRF6, LGALS4, OTOP2, DQX1, FUT3, XDH, NXPE1, SLC9A2, PROM2, MAL2, IGSF9, LIPH, HNF4A, RAB25, CLCA4, SERPINB5, PIGR, HEPACAM2, CCDC64B, GGT6, MS4A8, SLC5A1, MYO1A, PRR15L, MYO5B, FUT2, C10orf99, FAM3D, AGR2, B3GALT5, PRR15, RP5-881L22.5, SPINK4, SLC39A5, CLDN8, PLS1, NOX1, HNF1A-AS1, RP3- 406A7.7, ANXA13, RP11-96D1.11, FABP1, EPCAM, PRKCG, CAPN9, PRAC1, RP11-665N17.4, LEFTY1, CLDN7, CYP2C9, CDX1, CHP2, TMPRSS4, AOC1, RP11-22C11.2, FOXA3, URAD, HNF4G, LDHD, C1orf106, POF1B, CCL15, JPH1, TSPAN8, AMN, CAMSAP3, MUC5AC, EFNA2, PLA2G10, GRB7, PI3, SLC44A4, CTD-2196E14.5, LCN12, TMC5, CEACAM7, KRT19, DSG2, EPHA10, AC083900.1, GDA, SEMA4G, SLC6A14, SCNN1A, HMGCS2, AC079602.1, AQP8, TINAG, COL17A1, KLK1, S100P, TMEM54, CNGA1, CLDN3, RP11-304L19.1, SLPI, AKR1B10, KRT20, CA1, SPINK1, RP11-797A18.4, MB, TFCP2L1, RP11-305L7.6, FRMD1, SPDEF, PTPRH, RP11-395B7.2, GPX2, RBBP8NL, GPA33, PDE11A, LINC00483, FZD5, DSP, CA12, ITLN1, NOS2, FFAR4, TMEM184A, SFN, CLRN3, MTIG E.Goblet C11orf52, RP11-120K24.5, RP11-43N5.1, RP11-542B15.1, CTD-2231E14.4, LGSN, RN7SKP127, NUTM2E, TBX10, SYTL5, RP11-363E7.4, RP11-143K11.1, TFF1, SCEL, RN7SL676P, FER1L6, SLC25A30-AS1, PCDH20, ANKRD36C, RP11-805124.1, FAM177B, MUC5AC, LINC00342, RP11-845C23.2, RP11-730K11.1, STXBP5-AS1, FRY-AS1, SYTL2, TFF2, SBF2-AS1, RASD2, RP11-757F18.5, AC011718.2, ZG16, MUC1, SYTL4, MUC2, LGALS9B, FAM101A, MLLT3, FFAR4, RP11-452L6.1, TCTEX1D4, RP11-574K11.28, LGALS9C, GPR153, CAPN8, SHH, ADM2, AC007382.1, RP11-167J8.3, LINC01022, SMIM6, MFSD4, GALNT5, TEP1, BCAS1, GPRIN2, SDR16C5, ASPHD2, ZG16B, AC009133.21, C4orD6, GAN, FCGBP, GAREM, LNX1-AS1, MUC4 E.Immature_Enterocytes F11, RP11-525K10.3, RP11-576122.2, CA1, WFDC12, RP11-164P12.3 E.Immature_Goblet RP11-7115.4, IGFALS, AC015849.13, CLCA2, GALNTL6, IL37, AC073133.1, PRKCG, ITLN1, RETNLB, SPINK4, TMEM210, DLGAP1, CLCA1, LA16c-425C2.1, LINC00238, CREB3L4, LRRC26, CHRNA3, GALNT8, RP11-234B24.2, CTD-2547H18.1, AGR2, WFDC2, KLK15, KLK1, LINC00261, GIF, ST6GALNAC1, LINC00570, REG4 E.Secretory C11orf52, HTR3C, KLK13, MIR7-3HG, PAX4, PAX6, RP11-43N5.1, TAS1R1, TNNI1, VWA5B2, HTR3E, B4GALNT4, PYY, SH2D6, INSL5, SCGN, SH2D7, GCG, TRPM5, FEV, CHGA, CRYBA2, GNG13, PRPH, SST, CCDC129, PCP4, TPH1, SCG3, LCN15, KLHDC7A, OGDHL, KCNH6, POU2F3, AZGP1, TAS1R3, EYS, CTD-2231E14.4, KCNJ6, RP11-131L12.2, INSM1, ALOX12B, RAB3B, NCMAP, CCSER1, SCG2, CYP3A7, CPB1, IL17RB, RFX6, RN7SKP127, RIMBP2, CTD-2410N18.3, NKX2-2, NEUROD1, TBX10, SYTL5, SLC25A30-AS1, CNIH2, SLC18A1, C11orf53, RP11-143K11.1, RP11-363E7.4, RP11-93B14.5, MAFA, NRTN, AVIL, TFF1, LINC00470, KCNQ4, ABCA13, SCEL, TREH, GPR153, FER1L6, BMX, SCG5, RN7SK, NEUROG3, PSTPIP2, TGM3, PCDH20, ANKRD36C, KLB, ATP2A3, MEGT1, RASSF6, RP11-805I24.1, KLK11, FAM177B, PAQR7, PROC, ATP8A2, RP11-809C18.4, AC023490.1, RP11-730K11.1, TM4SF5, CACNA1A, HMX2, IGSF21, ADH6, SYTL2, TNNC1, RTBDN, PRSS22, FRY-AS1, GFI1B, FOXP4, RASD2, FAM101A, HOTAIRM1, AGAP1-IT1, HIP1R, SYT7 E.Secretory_All EYS, KCNH6, LINC01022, NEUROG3, TNNI1, VWA5B2, CRYBA2, HTR3E, SCGN, B4GALNT4, SH2D6, FEV, GCG, CHGA, PRPH, SH2D7, TRPM5, GNG13, RIMBP2, AC009133.21, ZG16, SLC18A1, LCN15, TPH1, SCG3, TBX10, RFX6, INSM1, SCEL, RP11-575A19.2, PKP1, MUC2, MUC5AC, BEST2, PCP4, KLHDC7A, REP15, TGM3, AC011523.2, TAS1R3, AC110619.2, SCG2, CTD-2231E14.4, RAB3B, RAD51AP2, POU2F3, CCDC60, AZGP1, KLK15, FCGBP, CCDC129, KLHL32, ALOX12B, ANO7, CLCA1, OGDHL, B3GNT6, KLK3, MB, ITLN1, TFF3, RN7SKP127, RETNLB, SNORA77, RAB26, CLCA2, NCMAP, KLK11, NKX2-2, KLK1, GALNT8, IL37, ANXA13, SPINK4, RP11-234B24.2, KLK12, TPSG1, CHRNA3, STXBP5-AS1, RAP1GAP, TMEM61, GPR153, IGFALS, TMEM210, SPDEF, CAPN9, SYTL5, SLC25A30-AS1, FOXA3, ABCA13, FFAR4, LRRC26, GALNTL6, LA16c-321D4.2, AGAP1-IT1, SYT7, TFF1, LINC00261, RP11- 363E7.4, SCG5, FAM177B, SCGB2A1, KLB, CCDC108, NRTN, GIF, PCDH20, LINC01001, ST6GALNAC1, WFDC2, TFF2, MLLT3, DNAJC12, ATP2A3, PRKCG, CREB3L4, CTD-2547H18.1 E.Secretory_TA ARHGAP36, DLX4, SIK3-IT1, RP11-430G17.3, RP11-363J20.1, SBSPON, RP11-231G3.1, RP11-396C23.4 E.Stem RGMB, SMOC2, PTPRO, LPCAT3, LGR5, LGR6, SNX32, RP11-760H22.2, C1orf95, RP11-21817.2, IZUMO2, NANOG, SLC22A11, SHISA6, RP11-219E7.4, HYDIN, RP11-2E11.9, SCN8A, TDRD6, MURC, GABRA4, PARD3-AS1, AC006159.3, RP11-645C24.5, AC068499.10, SERHL, RP1-20N2.6, RP11-130C19.3, FNDC5, RP11-132A1.4, RP11-268P4.4, LINC00924, RN7SL215P, AC078883.4 E.Tuft KRT18, SH2D6, AZGP1, LRMP, HCK, IFI6, PTPN18, PTGS1, AVIL, ATP2A3, GNG13, TRPM5, PLCG2, BMX, EIFIB, LUC7L3, MATK, BIK, HOTAIRM1, IL17RB, PSTPIP2, ANXA13, SH2D7, AKAP9, HTR3E, DEFB1, RASSF6, PPAP2C, IL13RA1, POU2F3, SPTLC2, SOX9, DPYSL3, IFT172, KLK11, COL27A1, CC2D1A, TREH, TMEM63A, TAS1R3, ZFHX3, CASP6, NCMAP, GRASP, MAP7, VAV1, C11orf53, CHDH, CCSER1, AFAP1L2, CD300LF, OGDHL, 7SK, HIP1R, DEGS2, LIMD1, CRYM, RP11-93B14.5, IGSF21, KCNQ1, GFI1B, SRGAP1, FAM171A1, PRSS22, LRP5, CCDC129, B4GALNT4, PIK3CG, PLCB2, PCP4, RALGAPA2, CTD-3094K11.1, MTSS1, PART1, KCNQ4, KLHDC7A, KDM4A, IRAK1, RN7SK, PAK3, SHB, hsa-mir-1199, FOXP4, ALOX12B, ADH6, CAMP, FUT6, NRTN, PHF12, U47924.27, PROX1, FHDC1, GANC, ZSWIM8, HOXA3, CCM2L, TNNI1, IGSF3, LRRC16A, ARHGEF5, COLCA2, HTR3C, KREMEN2, ARHGEF38, ATP8A2, HMX2, SHF, FAM229A, ABCB9, GKAP1, MADD, KLK13, AC023490.1, TRHDE, ARHGEF11, CEACAM19, RP11-285F7.2, TMEM191C, PAQR7, TAS1R1, TBC1D32, FMN1, USP35, GDPD1, RP11-440L14.1, RP11-1220K2.2, C2orf15, RP1-140A9.1, LINC01001, CDH26, AMER1, SHROOM2, LINC01071, RP11-72M17.1, HIST1H4A, HOXA1, ZNF490, RP1-199J3.7, PLA2G4D, TMEM211, RP11- 298I3.4, RP11-219G17.4, CABP4, RP11-712L6.5

TABLE 5 Immune Healthy specific markers for indicated cell types B.Bcells CDH15, CR2, CTB-43E15.4, GH1, GLDC, GPRC5D, HBD, HTR3A, IGHE, IGLJ2, IGLV3-12, IGLV5-48, NLRP7, OSTN-AS1, PAX5, RP1-148H17.1, RP11-1084E5.1, RP11-164H13.1, RP11-297B17.3, RP11-301L8.2, RP11-390F4.6, RP4-536B24.4, RP5-921G16.2, SERPINA9, SLC22A31, TRIM55, TSHR, UBE2QL1, ZC2HC1B, FCRLA, IGLL1, TCL1A, IGHD, IGLC2, RP5-887A10.1, FAM92B, CD19, MS4A1, VPREB3, IGKC, AL928768.3, IGHM, IGHA2, IGHG1, CD79A, IGHA1, IGHG2, IGLL5, IGLC7, AC104699.1, MZB1, IGJ, BANK1, CTA-250D10.23, DERL3, RP11-693J15.5, hsa-mir-5195, AC096579.7, TNFRSF17, IGHG3, WT1-AS, MIXL1, IGLV3-1, IGLV6-57, IGLV1-40, IGLV2-8, IGLV2-14, FGF23, IGLV2-11, IGLV3-16, FCRL5, LMTK3, AMPD1, IGLV1-47, TNFRSF13C, AF127936.3, FAM129C, AC104024.1, IGHV1-24, IGLV5-45, IGLV3-21, PKHD1L1, FCER2, AC096579.13, IGLV8-61, E2F5, IGKV1OR2-108, IGLV3-25, RP11-1070N10.3, IGLV3-10, KIAA0125, MEF2BNB-MEF2B, AC079767.4, CCR10, RP11-492E3.2, RP11-325K4.2, MYL2, RP11-138I18.2, IGLV2-23, IGLV4-60, EAF2, RP11-290F5.1, AP001058.3, CNR2, FCRL2, RP11-77H9.8, IGLV1-51, SSR4, CD79B, BLK, IGKV2D-28, IGLV3-9, P2RX5, AICDA, MEF2B, IGLV3-19, CRYBA4, AC096559.1, UBE2J1, RP11-16E12.2, AC007386.2, TEX9, ESR2, RAB30, IGKV4-1, SNX29P2, TXNDC5, RP3-402G11.25, IGKV1-12, IGLV10-54, IGKV1-5 B.Cycling MIOX, HBD, IGLV3-9, HIST1H1B B.FO COL19A1, RP5-887A10.1, FCRL4, IGHE, OSTN-AS1, GYLTL1B, SIDT1, BANK1, TNFRSF13B, IGHD, SELL, TEX9, CCDC50 B.GC RP11-485G7.5, RP11-624C23.1, RP11-138I18.2, SERPINA9, ANK1, C7orf10, HTR3A, RP11-511B23.1, BACH2, RP1-148H17.1, AC023590.1, IGKV6D-21, DBNDD1, AICDA, ANKLE1, BCL7A, TCL6, TRIM55, RP11-164H13.1, RP11-160H22.5, EYA3, BFSP2, SNX29P2, RP11-558F24.4, RP11-1070N10.3, CCDC144A, TCL1A, ACY3, RP11-960L18.1, NEIL1, WDR66, P2RX5, STAG3, GPR114, RPRD1B, HCAR1, SYVN1, IL21R, SMIM14, KLHL6, SEL1L3, TPD52, TERF2, TRIM59, TIGD1, RP4-739H11.4, BCAS4, LIMD2, LSM10, STAP1, MTMR14, CD180, RP11-16E12.2, GGA2, TNKS2-AS1, STX7, HMCES, DCAF12, MBD4, FBXO16, CD79B, FCRLA, STRBP, IQCB1, NGLY1, PARN, ST6GAL1, FCRL3, DEF8, TCEA1, TMEM156, CD53, RRAS2, NCF1, ZNF296, TOR3A, CD72, RFC1, EPS15, CYB561A3, LYPLAL1 B.Plasma IGLC3, IGLC7, FGF23, IGLV6-57, IGLV1-40, IGLV2-11, IGLV2-23, IGLV1-51, RP11-492E3.2, PSAT1, IGLV4-69, IGLV3-25, IGLV7-43, LINC00582, IGLV3-10, IGLV8-61, DNAAF1, IGLV10-54, IGLV5-45, IGLV4-60, IGLV3-16, CDH15, SLC22A31, IGLV1-50, RP11-1084E5.1, IGKV1OR2-108, ZC2HC1B, GH1, IGLV3-12, AF127936.3, LINC00525, UGT3A2, IGHV3OR16-9, NLRP11, RNF148, RP11-428K3.1 I.Immune AC004791.2, AC013264.2, AC104820.2, APOC2, ASGR2, ATP6V0D2, BTLA, CA10, CASS4, CATSPER1, CCL18, CCL3L1, CCL4L1, CCL4L2, CD180, CD1E, CD207, CD226, CD28, CD300C, CD300LB, CLEC4E, CLEC4F, CLEC9A, CLECL1, CRHBP, CTLA4, CXCR5, ELAVL4, FAM92B, FCER2, FCGR1A, FCGR1B, FCGR3A, FCN1, FCRL1, FCRL6, FCRLA, FLT3, FPR1, GAPT, GCSAM, GPR34, GPR84, GPRC5D, ICOS, IGHD, IL17A, IL18RAP, IL21R, IL22, ITGAX, JAKMIP1, KIR2DL3, KIR3DL2, KLHDC7B, KRT81, KRT86, LAMP3, LILRA2, LILRA3, LILRA5, LILRB2, LILRB5, LRRC25, LTA, MSR1, NLRC4, NLRP7, OSTN-AS1, P2RY13, PGLYRP2, PIK3R6, PKD2L1, RP11-18H21.1, RP11-291B21.2, RP11-327F22.2, RP11-354E11.2, RP11-365O16.3, RP11-367G6.3, RP11-542M13.3, RP11-556E13.1, RP5-1091N2.9, RP5-899E9.1, S100Z, SIGLEC1, SIGLEC12, SIRPB1, SNAI3, TBX21, TFEC, TIFAB, TNFRSF9, TNFSF8, TRAV4, UBASH3A, ZNF683, RUNX3, CD1C, FASLG, CD160, GZMK, TRDC, CD3D, XCL1, CTSG, CD3E, AC092580.4, TRGC1, TRBC2, KLRB1, TIGIT, CD300A, TPSAB1, IFNG, CD8A, GZMA, SNX20, SH2D1A, CST7, CD52, CCL4, CD247, XCL2, CD2, CCL5, DOK2, GZMB, TMIGD2, GZMM, TRAF3IP3, GNLY, NKG7, SIRPG, THEMIS, CD3G, CD7, ADORA3, MPEG1, KRT1, HCST, PLD4, LTB, TRGC2, IL2RB, SIT1, MAP4K1, RGL4, P2RY10, PTPRC, NCKAP1L, GRAP2, CSF2, CD37, CXCR6, S100A9, GPR18, SLA2, TNFSF14, CTSW, AMICA1, PRF1, ARHGAP9, GPR171, CD86, TBC1D10C, MARCH 1, SAMSN1, GPR183, LCP1, BCL2A1, SDS, RASGRP1, CD5, CMA1, TNFAIP8L2, HDC, LINC00402, FCER1A, IL1B, RP11-455F5.5, STAT4, CD244, IL7R, CD19, ARHGAP30, PCED1B-AS1, KLRD1, TRAT1, PTPN22, KLRC1, GZMH, AC109826.1, CCR5, LINC00996, PARVG, MS4A6A, TNIP3, CD48, NCR3, ITGAM, VPREB3, RNASE6, LCK, FPR3, GNA15, LY86, SASH3, CRTAM, MS4A4A, C1QB, LAPTM5, NCF1, WAS, HOPX, IGHV1OR15-1, CD6, FAM159A, APOBEC3H, CACNA2D3, IGSF6, IKZF1, LY9, CYTIP, MIR142, CSF1R, EVI2A, DUSP2, BFSP2, HLA-DOB, PTPRCAP, PTPN7, SPI1, RHOH, TLR10, CSF3R, TNF, FCER1G, BTK, MYO1F, AC020571.3, CHRM3-AS2, GPR65, CD53, CXCR3, C1orf162, SPN, ITGAL, TXK, CCL3, ADAM8, TCL1A, AIF1, CD96, KLRC2, PDCD1, CPA3, MYO1G, IL10RA, HAVCR2, LILRB4, MMP12, CD40LG, SCIMP, CSF2RA, EVI2B, TREM2, LINC00892, TREM1, DOCK2, EMB, PILRA, CYBB, RGS1, MS4A7, CHI3L2, RP3-522D1.1, C1QC, IL8, KCNA3, SLFN12L, CARD11, CD69, PYHIN1, ITK, LAT2, CORO1A, DNASE1L3, ITGB2, GPR132, KLRG1, RP11- 190C22.9, LAIR1, FGD3, SCML4, BLK, SLC18A2, LRRN3, CD8B, FAM26F, PLA2G7, CLEC10A, CD209, C5AR1, SLAMF8, SP140, TESPA1, CD200R1, PRAM1, CXorf21, VSIG4, SKAP1, LPXN, C1orf186, SYTL3, CD163, IFI30, WDFY4, SH2D2A, RP6-91H8.3, RP11-94L15.2, LST1, CD79A, CD27, HLA-DQB2, LYZ, DENND1C, CD70, RP11-222K16.2, CYTH4, RASSF5, CLEC2D, SH2D1B, CLEC4A, C1QA, MS4A1, CCR2, OSCAR, C3AR1, CD101, BATF, ACAP1, CD33, IGLC2, RP3-477O4.14, CD38, CSTA, PIM2, IL4I1, OSM, MMP9, SLAMF7, NCF2, RP11-489E7.4, IFNG-AS1, ITGB7, IL1RN, ZAP70, ITGB2-AS1, STK17A, DUSP4, RP11-693J15.5, FAIM3, FAM179A, CD83, TMEM156, IGLL5, DAPP1, IGFLR1, SLAMF1, CXorf65, RAC2, BIN2, F13A1, C1orf61, OLR1, SAMD3, IGKC, KYNU, AL928768.3, ZNF331, TNNI2, TLR7, OXNAD1, IGLC7, IL16, TAGAP, SLAMF6, WNT10A, P2RY6, NLRP3, KCNAB2, KMO, APBB1IP, CCR1, CD72, RASAL3, EVL, LAT, LIMD2, CREM, POU2F2, ADPGK-AS1, UPK3A, SLC7A5, TNFAIP3, TLR2, HLA- DQA1, SELL, HCLS1, IL23A, AC017104.6, TRAC, GHRL, IRF4, RELT, SEPT1, HLA-DQB1, FAM46C, AC006129.4, TMC8, AP001058.3, SNX10, PLEK, IGHG1, PNOC, LINC00528, CD84, STAP1, IGJ, FGD2, FAM49B, CTA-384D8.34, HENMT1, RGS18, PARP15, MNDA, PHACTR1, P2RY11, EBI3, MZB1, YPEL5, FMNL1, STK4, AOAH, COTL1, MMP25, RP11-324I22.3, SPNS3, IL2RA, PKHD1L1, GATA3, DUSP10, TNFAIP8, SLA, MYBL1, RAB33A, EAF2, FGF23, P2RX5, CRLF3, HLA-DPB1, SEPT6, ARL4C, GPR114, UTS2, RP11-70C1.1, IGLL1, DENND2D, LCP2, RGS19, ARRB2, CLIC3, TYROBP, AIM2, RORA, TC2N, RP11-539L10.2, PDE4B, RP11-347P5.1, IL2RG, PRMT10, PIK3CD, TNFRSF18, SIGLEC10, IL1RAPL1, NCF4, GLIPR1, SMAP2, RP11-863P13.3, CKLF, IGHG2, GALR2, TRAF1, HLA-DRA, ICAM3, PRR7, PRKCB, MAP3K8, PIK3AP1 I.Lymphoid AC013264.2, AC104820.2, CA10, CR2, CXCR5, DTHD1, GPRC5D, IGHD, IGLV5-48, IL22, JAKMIP1, KIR3DL2, KRT81, KRT86, LINC00861, NCR2, NLRP7, OSTN-AS1, RP11-18H21.1, RP11-291B21.2, RP11- 403A21.2, RP11-664D1.1, TBX21, TRAV4, ZNF683, CD160, XCL1, XCL2, GZMK, AC092580.4, TIGIT, GZMA, TRGC1, GNLY, CD3D, IFNG, CD3E, CD2, CD7, CCL5, IL2RB, TRGC2, CD3G, RASGRP1, TRDC, CD247, CD8A, IL18RAP, CXCR6, KLRB1, GZMM, TRBC2, FCRLA, PRF1, KLRC1, VPREB3, ICOS, TRAT1, KLRD1, SIRPG, GZMH, LCK, LINC00402, SLA2, IL17A, HOPX, IGHV1OR15-1, KLRC2, SIT1, FASLG, RGL4, BLK, CHRM3-AS2, CD96, TMIGD2, CD40LG, LRRN3, CD6, PYHIN1, NKG7, SH2D1A, CHI3L2, RP11-542M13.3, TXK, IL7R, SCML4, TCL1A, UBASH3A, IGLL5, THEMIS, FCRL6, SH2D1B, RP11- 222K16.2, CD8B, MS4A1, GZMB, STAT4, CD79A, CD27, SLFN12L, SH2D2A, CD70, TNFSF14, IGHG3, IGLC2, CLEC2D, AC017104.6, CD19, IGLL1, FAM179A, RP11-94L15.2, FAM92B, FAM159A, SLAMF1, ZAP70, CD244, RP11-553L6.2, RP11-489E7.4, C1orf61, CD5, PGLYRP2, SLAMF6, PTPRCAP, RP11-284N8.3, IFNG-AS1, AL928768.3, CD28, IGJ, IGKC, SMKR1, GPR171, IGHG1, SAMD3, TRAC, EVL, GAT A3, IL23R, LTA, IGHA2, MZB1, AP001058.3, BCL11B, P2RX5, IGHA1, ITK, PARP15, APOBEC3H, CARD11, TBC1D10C, PCED1B-AS1, AC069363.1, CCR7, LINC00426, RP11-539L10.2, STK17A, TC2N, TPRG1, RP11- 279F6.3, CLIC3, CXorf65, IGLC7, AC104699.1, SEPT1, TNFRSF18, AC078883.3, TNFRSF13B, IL2RG, IGHG2, POU2AF1, PLCH2, RORA, MYBL1, CD52, ACAP1, CTLA4, FAM46C, GPR18, DERL3, CACNA1C- AS2, PTPN4, RP11-693J15.5, CCDC65, DEN D2D, ESR2, LTB, TNFRSF17, IGLV2-14, S1PR4, FGF23, NCR3, MIXL1, SPOCK2, OXNAD1, CCR5, AC096579.7, NUGGC, WT1-AS, PKHD1L1, PCED1B, RCAN3, CTSW, KLHDC7B, PARP8, ANKRD44-IT1, FKBP11, SYTL1, TAGAP, PPP1R18, IGLV5-45, ZBP1, EMB, TNFRSF13C, LINC00649, PRKCQ-AS1, FAIM3, RP11-277L2.4, AAK1, P2RY11, GRK6, SPINK2, CYTIP, SASH3, ORMDL3, FYN, LEPROTL1, PTPN22 M.CD69neg_Mast NTRK1, IL9R, ADAM22, CATSPER1, FAM21B, ABCB8, NSMCE1, AJ271736.10, ARHGEF6, FECH, ACLY, NCOA4, UBA7, BRAP, KRT1, FAM212A, MAML1, SLC43A3, SAMSN1, LPCAT2, GMPR, SPACA3, LTC4S, HPGDS, HSD17B12 M.CD69pos_Mast ADCYAP1, CALB2, RP11-501J20.5, TPSD1, IL13, RP11-557H15.4, IL1RL1, RP4-794H19.2, ARL5B-AS1, RP11-705O1.8, AF213884.2, IL1RAPL1, DKFZP434E1119, IL5RA, ENPP3, PPP1R15A, NFKBIZ, FER, AC020571.3, HDC, FAM46A, EGR3, ANXA1 M.Cycling SYCE2, ZMYND10, FAM72C, CDC25B, HTR7, SIGLEC15, CDK1, TUBA1B, KPNA2, HJURP, COQ2, FAM64A, H2AFZ, TPK1, RAD51AP1, RP11-556E13.1, TROAP M.DCs BAI1, CD1B, CTD-2514K5.2, RFPL4A, RP11-117D22.2, RP11-667K14.3, RUFY4, XCR1, SFTPD, TMEM170B, FLT3, UPK3A, SLAMF9, FAM230A, CLEC4F, NAMPTL, CLEC9A, CD207, RYR1, TBX19, CD1E, CTD-2619J13.17, CX3CR1, SERPINF2, INHBA-AS1, CD1C, CPVL, CTD-2319I12.1, FAM46B, RP11- 248J18.2, HLA-DQB2, MYCL, LEKR1, NME8, CD1D M.Macrophages AC005082.12, LILRA6, RN7SL138P, GRIN2D, AZU1, KCNC3, SIGLEC11, SLC7A8, FABP3, PLA2G2D, SLC40A1, RP3-414A15.10, FOLR2, CRHBP, TREM2, OTOA, HSD17B14, RP11-848P1.2, RNASE1 M.Mast ADCYAP1, AMHR2, CALB2, GATA1, GCSAML, MS4A2, NTRK1, RP11-501J20.5, TPSD1, XXbac- BPG13B8.10, IL1RAPL1, ST8SIA6, C1orf186, TPSAB1, RP11-354E11.2, IL13, RP11-557H15.4, SLC45A3, HDC, SLC18A2, CMA1, AC004791.2, SIGLEC8, SVOPL, IL1RL1, CPA3, CTSG, MAOB, KRT1, VWA5A, GATA2, RP4-794H19.2, CTD-3203P2.2, RAB27B, LTC4S, ATP6V0A2, ARL5B-AS1, SPACA3, RP11- 705O1.8, HS3ST1, AF213884.2, ADRB2, DKFZP434E1119, LEO1, MITF, IL5RA, CTNNBL1, SMYD3, ENPP3, TIAM2, PPP1R15A, VWC2, NFKBIZ, FER, AC020571.3, GMPR, CAPG, TESPA1, BTK, FAM46A, UBXN10, PLIN2, RP11-169D4.2, CRBN, ANXA1, ALS2, BACE2, LMO4, GLUL, RP11-443B7.1 M.Monocytes FTL, HLA-DRA, HLA-DRB1, HLA-DPB1, CST3, SAT1, HLA-DPA1, GPX1, AIF1, HLA-DQA1, LYZ, HLA- DQB1, HLA-DRB5, RNASET2, C1QA, HLA-DMB, TYMP, MS4A6A, C1QC, CTSS, DNASE1L3, C1QB, CTSB, SPI1, CTSZ, CPVL, IGSF6, PLAUR, MS4A7, FAM26F, HLA-DQA2, RNASE6, HLA-DQB2, LGMN, IL1B, CLEC10A, FUCA1, IFI30, BID, LGALS2, MPEG1, SLC40A1, VSIG4, STAB1, SDS, MS4A4A, CD68, FCGR2A, MNDA, IL8, PLA2G7, CSF1R, RB1, GM2A, CECR1, CD86, ADORA3, HBEGF, P2RY6, ADAP2, FOLR2, CSF2RA, MMP12, C5AR1, SLAMF8, HLA-DOA, AP1B1, CFP, SLC31A2, G0S2, VMO1, PILRA, S100A9, CD209, TTYH3, NAIP, LILRB4, CLEC7A, CD163, FPR3, TREM2, IL18BP, NCF2, CLEC4A, CLEC9A, ATP6V0D2, NUP214, OTOA, RAB42, LILRB5, CXCL3, LRRC25, CMKLR1, EBI3, P2RY13, FCGR1A, SLC7A8, CACNA2D3, LILRB2, CD1E, EMILIN2, SIGLEC1, RN7SL368P, CSF3R, BATF3, MYCL, DAPK1, TRPM2, CSTA, IL1RN, CRHBP, CD300C, RGS18, OLR1, RP11-426C22.5, TREM1, LY96, RP11- 365O16.3, RP3-522D1.1, TIFAB, RP11-1143G9.4, PKD2L1, CCL18, TLR2, HCAR2, ITGAX, MSR1, ASGR2, F13A1, CLEC4G, FLT3, FCN1, RP11-290F20.3, OSCAR, LILRA2, GHRL, CD207, HCAR3, RP3-399L15.3, APOC2, RP5-899E9.1, RP11-863P13.3, CCL3L3, CLEC4E, LILRA3, RP11-556E13.1, FCGR1B, CCDC170, GPR84, RP11-760N9.1, CD300LB, ELAVL4, S100A8, GALR2, CLEC4F, FPR1, NLRC4, RP11-472N13.3, LILRA5, C19orf59, GSDMA, INHBA, GRIP1, RP11-426L16.8, SFTPD, RP11-190C22.9, ALOX15B, MRC1L1, TLR8, XCR1, UPK3A, SYCE2, RP11-680A11.5, CD1B, LILRA6, MS4A14, SLAMF9, CX3CR1, IL27, KCNK13, RNASE2, RP11-701P16.5, GRIN2D, RP11-848P1.2, AC005082.12, RYR1 M.Myeloid AC004791.2, AC011899.9, AMHR2, ASGR2, ATP6V0D2, CALB2, CD300LB, CLEC4E, CLEC4F, ELAVL4, FCGRIA, FCGRIB, FCN1, FPR1, GATA1, GCSAML, GPR84, INHBA, LILRA3, LILRA5, LILRB2, LILRB5, MS4A2, NLRC4, RP11-365016.3, RP11-472N13.3, RP11-556E13.1, RP11-760N9.1, RP5-899E9.1, S100A8, SIGLEC12, SIGLEC8, TIFAB, XXbac-BPG13B8.10, CTSG, CLEC9A, CMA1, SLC18A2, P2RY13, RP11- 557H15.4, CDIE, SDS, MSR1, FPR3, MS4A4A, MS4A6A, KRT1, CSF1R, ADORA3, IGSF6, S100A9, MMP12, IL1B, TREM2, C1QB, FCER1A, C1QC, CD209, CACNA2D3, PLA2G7, CD163, RP3-522D1.1, TPSAB1, AIF1, CSF3R, CD207, DNASE1L3, PKD2L1, C1QA, C5AR1, SIGLEC1, IL1RAPL1, HDC, F13A1, LILRB4, VSIG4, IL8, CLEC10A, MS4A7, LYZ, CSTA, C1orf186, CCL18, SVOPL, TREM1, SFTPD, OSCAR, RP11-190C22.9, TLR2, CSF2RA, IL1RN, CRHBP, RP11-354E11.2, IL13, CPA3, OLR1, P2RY6, SLC45A3, APOC2, LILRA2, PILRA, RAB42, CFP, RASGRP4, FLT3, MNDA, CPVL, MPEG1, IFI30, GSDMA, STAB1, RP11-426L16.8, LRRC25, CCL3L3, CD68, RP11-76E17.3, GALR2, MAOB, LINC00884, CD300C, SLAMF8, IL10RB-AS1, NCF2, RP11-1143G9.4, FAM26F, HCAR3, VWA5A, FTL, HS3ST1, FUCA1, GM2A, SLC40A1, RNASE6, HLA-DPB1, FOLR2, CLEC4A, GLUL, GRIP1, CD86, IL18BP, RP11-426C22.5, ALOX15B, HLA-DRB1, PIK3R6, RP11-42110.1, RGS18, LY96, FCGR2A, GATA2, RP11-70C1.1, GHRL, CST3, CASS4, TBXAS1, HLA-DPA1, CTD-3203P2.2, CXCL16, C19orf59, TNFAIP8L2, TNNI2, HLA-DQA1, HLA-DRB5, PLAUR, RNU1-60P, RAB27B, TTYH3, VMO1, ATP6V0A2, CD33, NUP214, TRPM2, RP11-863P13.3, DAPK1, CTSS, CTSB, SGK1, ARL5B-AS1, HCAR2, CMKLR1, OTOA, RENBP, ATP6V1F, NCF4 M.Neutrophils S100A8, RP11-701P16.5, S100A9, FCN1, EREG, NLRP3, CSTA, APOBEC3A, G0S2, TLR2, C5AR1, LILRB2, OLR1, FCGR1A, EMILIN2 M.Tissue_DCs CDIB, CTD-2514K5.2, RFPL4A, RP11-117D22.2, RP11-667K14.3, SFTPD, TMEM170B, SLAMF9, FAM230A, CLEC4F, NAMPTL, CD207, RYR1, TBX19, CD1E, CTD-2619J13.17, CX3CR1, INHBA-AS1, CD1C, GHRL, RP11-248J18.2, LEKR1, NME8, TMEM52B, CD1D, MS4A14, PLD4, FCER1A, CACNA2D3 M.Tolerogenic_DCs XCR1, CLEC9A, CTD-2319I12.1, CLCN4, FBXO27, DGAT2, IDO1, BATF3, WDFY4, FLT3, SERPINF2, FKBP1B, DSCAML1, CPNE3, SNX3, PPM1J, RP11-661A12.7, CPVL, KIAA1598, KIAA0226L, C1orf54, FNIP2, C8orf47, TNNI2, TACSTD2, TOMM34, UCP3, VAC14 T.Activated_CD4_loFos AC006369.2 T.CD4 CTLA4, LAIR2, RP11-664D1.1, ATG9B, CD40LG, IL17A T.CD8 CD8B, RP11-291B21.2, DRAXIN, CD8A T.CD8_IELs TRBV20-1, RP11-535A5.1, PAGE5, KLRC2, NCR2, TRGC1, TRGC2, DRAXIN T.CD8_LP RP11-291B21.2, CD8B T.CXCR6_Th17 RP11-85K15.2, IL12RB1, CCL20, SLAMF1, KLRB1, ZFYVE28 T.Cycling_T ABCD2, CCT6B, C11orf82, C16orf59, A1BG, C5orf17, ZNF682 T.ILCs LINC00299, TNFSF11, IL23R, SPINK2, SLC4A10, SAMD10, OTUD5, TRGV9, RP11-425D10.10, IL4I1, LINC00176, ALDOC, FXYD7, CASP3, AREG, KRT86, HINT3, CSF2, PRMT10, LTA4H, FAM167A, ZNF385C, PDZK1, MED30, ZMYM2 T.MT FSCN3, BZRAP1, AP000350.4, AC132872.2 T.Memory_CD4 RP11-664D1.1 T.NK PADI4, SPTSSB, KLRF1, RP11-401F2.3, BCO2, SH2D1B, EOMES, XCL1, XCL2, KLRC1, IL2RB, CLIC3, FGR, RP11-222K16.2, AC069363.1, NKG7, GZMB, KLRD1, AC017104.6, PRF1, GEMIN5, EIF3G, FCGR3A, CMC1, GNLY, B3GNT7, CHST12, APOBEC3G T.PD1_CD4 RP5-1028K7.2, NMB, CD200, KIF2A, PDCD1, MPP7, RP11-455F5.5, PVALB, CDK5R1, PRKRIR T.Tcells CA10, CPA5, FOXP3, RP11-664D1.1, TRAV4, RP11-291B21.2, IL2, IL17A, LINC00402, BCL11B, CD8B, CD3G, CD3D, CTLA4, AC104820.2, CD5, RP11-279F6.3, CD6, CACNA1C-AS2, CD28, CCDC65, TRAT1, TRGC2, SIRPG, GPR171, LINC00649, CD8A, CD3E, FAM115C, TRAC, ACSL6, TNIP3 T.Tregs RP11-316P17.2, LAIR2, MCF2L2, ANKS1B, FANK1, FOXP3, RP11-580116.2, DUSP16, TRAV8-2, TNFRSF9, IL10, BATF, CTLA4, RP11-382J12.1

TABLE 6 Immune UC specific markers for indicated cell types B.Bcells AC007381.3, AC007880.1, AC073072.5, AC104699.1, AL109761.5, AP005530.2, BEND4, C7orf72, CCL25, CHIA, CHIT1, COL19A1, COL24A1, CTB-43E15.4, FAM92B, GPRC5D, HCFC1-AS1, IGHE, IGKV1D-43, IGLV5-48, LINC00494, LINC00582, LINC00643, LRRC4, MYF6, OVOL3, RP1-148H17.1, RP11-138I18.2, RP11-203B7.2, RP11-297B17.3, RP11-301G19.1, RP11-301L8.2, RP11-390F4.6, RP11-428G5.5, RP11- 493L12.3, RP11-511B23.1, RP11-624C23.1, RP11-625L16.3, RP11-689B22.2, TREML2, UBE2QL1, UGT3A2, UTS2B, hsa-mir-5195, hsa-mir-5571, HTR3A, IGLL5, IGLC3, CR2, IGLC2, SERPINA9, MED12L, MS4A1, CLEC17A, AC104024.1, AC096579.13, IGHG2, RN7SL17P, IGHA2, PAX5, IGLC7, CD19, IGKC, AL928768.3, AC096579.7, IGHA1, TCL1A, FCRLA, DERL3, IGHD, IGLL1, VPREB3, DKK1, MIXL1, IGHG1, MZB1, WT1- AS, IGHG4, IGLV3-16, FCRL5, IGLV6-57, LINC00525, RP5-887A10.1, BLK, FCER2, RP11-159H10.3, PKHD1L1, TNFRSF17, IGJ, FGF23, NLRP7, RP11-290F5.1, AC009473.1, TNFRSF13C, OSTN-AS1, CD79A, MRVI1-AS1, AF127936.3, FAM129C, IGLV1-40, IGLV2-11, MYL2, RP11-693J15.5, CD79B, IGLV10-54, WDR66, CTD-2306M10.1, FCRL1, IGLV3-1, IGKV2D-30, RP11-485G7.5, AC096559.1, IGHV1-24, KIAA0125, RP11-1070N10.3, AICDA, CD72, C7orf10, BANK1, RP11-492E3.2, DNAAF1, SNX29P2, RP11- 480C16.1, EAF2, CLECL1, PNMA6C, IGLV3-25, HVCN1, CRYBA4, BLNK, FCRL4, CD180, AC023590.1, MEF2BNB-MEF2B , IGKV1-6, SPAG4, CCDC144A, AC007386.2, ZCCHC7, IGKV2-30, UBE2J1, AMPD1, NEIL1, POU2AF1, FCRL2, HBD, SSR4, RP11-960L18.1, IGKV5-2, RP11-16E12.2, XBP1, IGKV1-12, TNFRSF13B, POU2F2, C12orf77, CTC-378H22.1, CD22, AP001058.3, ESR2 B.Cycling C7orf72, GLT1D1, RP11-301G19.1, STK4-AS1, ZNF730, BTN1A1, CTD-2561J22.5, AKAP2, RP13-494C23.1, RP11-553K8.2, CTC-332L22.1, KCNQ5-IT1, KLLN, RP11-286H14.6, SNORA70, CENPI, STOX1, C6orf99, RP13-20L14.6, RP11-449H11.1, IGHE, WDR76, C11orf65 B.FO AC002480.5, CCDC78, RP11-444D3.1, COL19A1, RP11-624C23.1, RP5-887A10.1, AC073072.5, RP11- 445F6.2, OSTN-AS1, WASIR2, UTS2B, AC007880.1, FCRL4, TNFRSF13B, CLECL1, RP3-455J7.4 B.GC RP11-567J20.3, RN7SL17P, LRRC4, SERPINA9, RP11-138I18.2, RP11-203B7.2, HRK, NEIL1, C9orf66, PUS10, NPAS1, AC096559.1, RP11-72I8.1, CD22, HTR3A, MIXL1, CD180, C7orf10, CCDC144A, SEMA4A, TRAF4, CD79B, USP6NL, KLHL14, RP11-960L18.1, RP11-542M13.3, IGF2BP3, IFNG-AS1, P2RX5, IL4R, ADORA2A-AS1, RP11-511B23.2, BFSP2, GPR18, RP11-307E17.8, AC023590.1, SMIM14, CYB561A3, SNX29P2, ESR2, GPR114, BCL11A, RP11-164H13.1, BCL7A, AP003419.16, CR2, CNR2, RP11-413H22.2, SYVN1, SYPL1, PLEKHF2, KMO, AMFR, RANBP2, ZNF581, RFTN1, SLC38A9, NCOA3, WDR66, BLNK, HLA-DOB, CD53, FCRLA, FAM105B, VNN2, CD40, AC145110.1, KIAA0922, RP11-158I9.5, ICOSLG, PXK, XKR6, RN7SL172P, VCPKMT, ITSN2, PKHD1L1, MS4A1, TMEM206, CPNE5, LIMD2, RP11-248J18.3, CD72, RAB30, RASGRP3, SYNGR2, MTMR14, GGA2, RNGTT, MGAT3, TMED8, SNX8, MOAP1 B.Plasma DCC, GH1, IGHJ2, IGKV1D-43, MYBPC2, MYF6, PRRG3, RP11-301L8.2, RP11-625L16.3, RP11-689B22.2, SCARNA16, TNN, TPTE2, TRIM55, UBE2QL1, UGT3A2, hsa-mir-5571, IGLV4-60, IGLV3-16, IGHG2, DKK1, IGLV1-40, AF127936.3, IGKV5-2, IGLV2-8, IGLV3-1, AC096579.7, IGLV6-57, IGHV1-24, FAM92B, IGHA2, DNAAF1, IGLL1, CTB-43E15.4, IGLV10-54, IGKV3-11, IGKV2D-30, AMPD1, IGHG3, PNMA6C, IGLC2, IGHG1, IGKV3-20, IGLV7-43, IGLV7-46, IGKV2-30, IGKV6-21, SPAG4, AL109761.5, IGLV9-49, IGLV3-25, IGLV2-11, IGKV1D-13, IGHG4, IGKV4-1, RP11-390F4.6, RP11-290F5.1, IGLC7, DERL3, SLC22A31, IGHA1, IGLV5-48, GPRC5D, IGKC, RP11-492E3.2, SSR4, IGKV1-6, JSRP1, IGLC3, IGJ, IGKV2- 24, IGLL5, XBP1, GUSBP11, LINC00582, RP11-554E23.4, FKBP11, IGHM, TNFRSF17, CHAC1, WNT10A, LINC00525, HERPUD1, LMTK3, IGKV3D-15, IGLV1-36, SEC11C, IGLV2-18, AC093818.1, IGKV1D-39, PDK1 I.Immune ABCD2, AC004791.2, AC011899.9, AC104699.1, AC104820.2, AC109826.1, AMPD1, AQP9, C11orf21, C19orf59, C20orf201, CA10, CASS4, CCL3L1, CCL3L3, CCL4L1, CCL4L2, CCR2, CCR5, CD1A, CD1B, CD226, CD300C, CD300E, CD300LB, CD80, CEACAM4, CLEC4E, CLEC4F, CLEC5A, CLEC9A, CMA1, CR1, CR2, CRYBB1, CSF3R, CTB-138E5.1, CTC-378H22.1, CTD-2337J16.1, DPEP3, EMR3, F5, FAM92B, FCGR1A, FCGR1B, FCN1, FCRL1, FLT3, FOXP3, FPR2, GPR141, HBD, HK3, IGHV1OR15-1, IKZF3, IL18RAP, IL22RA2, IL26, IL2RA, JAKMIP1, KCNK13, KRT1, LILRA1, LILRA2, LILRA3, LILRA4, LILRA5, LILRA6, LILRB2, LINC00402, LINC00582, LRRN3, MARCO, MEFV, MS4A14, MSR1, NLRC4, OSTN-AS1, P2RY13, PGLYRP2, PIK3R6, PKD2L1, PTCRA, PVALB, RASGRP4, RETN, RN7SL138P, RNASE2, RP11- 1381I8.2, RP11-169D4.2, RP11-265P11.2, RP11-291B21.2, RP11-297B17.3, RP11-316P17.2, RP11-354E11.2, RP11-365O16.3, RP11-367G6.3, RP11-403A21.2, RP11-472N13.3, RP11-542M13.3, RP11-556E13.1, RP11- 701P16.5, RP11-737O24.5, RP11-76E17.3, RP11-798K3.3, RP11-8L8.2, RP11-960L18.1, RP5-1091N2.9, RP5- 899E9.1, RYR1, SIGLEC1, SIGLEC12, SIGLEC14, SIRPB1, SUCNR1, TCHH, TFEC, TIFAB, TLR8, TNFRSF13C, TNFSF8, TRAV4, TREM2, ZFP57, ZNF831, PLD4, FPR1, CD1E, FASLG, OSM, RUNX3, CD1C, KLRB1, GCSAM, GZMH, ITGAX, CD86, LINC00892, C3AR1, CD207, CHRM3-AS2, IL17A, DOCK2, CTLA4, BTLA, CLECL1, HCST, NKG7, NLRP3, FCER1G, CXCR6, CD3D, RP5-1028K7.2, CD247, CD2, SIRPG, GPR34, CCL5, CD52, HDC, AIF1, CD28, GZMA, XCL1, HTR3A, TRDC, FOLR2, SDS, LRRC25, SIT1, SPI1, SH2D1A, UBASH3A, MS4A6A, CD3E, DOK2, CXCR5, THEMIS, C1QA, GPR18, LY9, FCER2, RGL4, AC013264.2, CCL3, MPEG1, STAP1, GZMM, CSF1R, PRF1, TIGIT, CST7, CD209, C1QC, TRGC1, SASH3, CCL4, IFNG, TRGC2, CD3G, CLEC10A, RP11-664D1.1, CTSG, NUGGC, AC092580.4, C1QB, P2RX5, S100A8, LCK, SAMSN1, CTA-250D10.23, TRAF3IP3, LST1, TIMD4, ZBTB32, RP11-164H13.1, GTSF1, ITGB2, PTPRC, IL1B, APOBEC3H, CD69, TXK, RP11-190C22.9, PLA2G7, GNLY, AMICA1, HAVCR2, ATP6V0D2, IKZF1, PTPRCAP, MMP12, MS4A7, XCL2, CD53, RP11-553L6.2, GZMK, C1orf162, TNFAIP8L2, TBC1D10C, IGSF6, LTB, IL22, FXYD7, CD40LG, IGHD, LILRB5, WAS, LCP1, NCR3, TPSAB1, LILRB4, MS4A4A, IGHG2, CYTIP, TRAT1, CD6, CD5, EVI2A, BTK, LAPTM5, TMIGD2, CACNA2D3, TRBC2, IGLL5, CD79A, RGS1, IGLC2, MS4A1, KMO, CYBB, IGHG3, FCER1A, GZMB, CD163, LY86, FAM26F, CD7, FPR3, AC079767.4, PCED1B-AS1, SNX20, CD180, ZAP70, CD300A, SP140, EVI2B, ITGB7, EBI3, NCF2, IFI30, MAP4K1, IGLC3, ITGB2-AS1, CSTA, FCGR3A, GPR183, OLR1, DENND1C, CSF2RA, CCL22, TNF, CD244, STAT4, LAIR1, GPR171, PDCD1, DNASE1L3, NCKAP1L, AC006129.4, NOD2, SERPINA9, RP11-455F5.5, RNASE6, CP A3, BCL2A1, TCL1A, PYHIN1, DUSP2, CD19, C12orf42, IL2RB, MIXL1, LTA, PARVG, CRTAM, CCL18, LAX1, CXorf21, FAIM3, NCF1, VSIG4, GAPT, GRAP2, SLC18A2, FGD2, BFSP2, CD160, TLR10, CD37, MIR142, PRKCB, RP11-693J15.5, RHOH, BLK, TNNI2, TYROBP, IGHG4, PAX5, LINC00861, CX3CR1, CLEC4A, CD38, FAM129C, AC020571.3, C16orf54, CORO1A, IGHG1, ITK, IFNG-AS1, GPR65, SPN, DNAJC5B, LAT2, P2RY10, F13A1, MYO1F, AGAP2, CCR7, TNFSF14, ADORA3, TMEM156, KLRD1, RIC3, BATF, CD8A, IL10RA, SLA2, CD48, ARHGAP30, IL10, SELPLG, ADAM8, RP11-637A17.2, CD84, SNAI3, AL928768.3, CD101, CATSPER1, SKAP1, IL16, HLA-DQA1, TBX21, HLA-DOB, CD96, RASGRP1, SLAMF6, CXCR3, CD22, SH2D2A, CTA-384D8.34, CD70, CD72, ARHGAP9, AIM2, PLEK, TESPA1, FCRL3, RP11-134P9.1, CYTH4, PTPN7, PTPN22, P0U2AF1, AC104024.1, IGKC, SLA, GPR132, MYO1G, STAC3, C1orf186, MZB1, RP11-493L12.4, RP11-284N8.3, PNOC, SLAMF7, FERMT3, PHACTR1, KLHDC7B, AP000783.1, SELL, UTS2, IL12RB1, CD8B, RASSF5, LINC00996, ITGAL, NCF4, AC096579.7, RASGRF1, CLEC2D, S100A9, IGHA2, GHRL, SERPINB9, IGLC7, SCML4, IGHM, CLEC12A, IGJ, AC096579.13, LYZ, HCLS1, TNFRSF18, SIGLEC10, RAC2, TAGAP, BIN2, LPXN, RASAL3, HCAR3, MYBL1, CD27, SLAMF8, ICOS, RP3-477O4.14, RP11-1143G9.4, SIGLEC7, GATA3, CARD11, CD200R1, PCED1B, CFP, BZRAP1-AS1, CTD-2514K5.2, KLRC2, FGD3, WNT10A, FCRL5, BCL11B, MARCH1, HLA-DPB1, SEPT1, IGLV6-57, MRC1L1, KBTBD8, RP11-158G18.1, EPHA1-AS1, KLRG1, GNA15, ACAP1, TNFRSF13B, FAM110A, HLA-DQB1, TRAC, AC104653.1, HAMP, HLA-DMB, TNFRSF17, BANK1, ATP8B4 I.Lymphoid AC002331.1, AC006369.2, AC104699.1, AL109761.5, AMPD1, C15orf53, C4orf26, CA10, CCL25, CCR6, DTHD1, F5, FAM179A, FAM92B, FCRL1, FOXP3, GPRC5D, IGHE, IGLV5-48, IL17F, IL2, IL26, JAKMIP1, KISS1R, KRT81, LINC00402, LINC00582, LRRN3, OSTN-AS1, RP11-104L21.3, RP11-222K16.2, RP11- 265P11.2, RP11-275I4.2, RP11-291B21.2, RP11-297B17.3, RP11-403A21.2, RP11-686F15.2, RP11-936I5.1, TRAV4, TRBV28, FASLG, XCL1, GZMH, RP5-1028K7.2, CHRM3-AS2, RP11-664D1.1, SIRPG, CD247, CCL5, IL17A, CXCR5, THEMIS, AC013264.2, SH2D1A, IGHV1OR15-1, CD3D, IFNG, GZMM, TIGIT, AC092580.4, LCK, GZMA, XCL2, HTR3A, CD3G, NUGGC, TRGC2, KLRB1, RP11-553L6.2, CD3E, FXYD7, TXK, LINC00861, CD40LG, CD6, GZMK, FCRL4, IGLL5, CD2, TRBC2, FCRL3, EOMES, ZAP70, TRAT1, AC104820.2, LTA, IGLC2, IGHG2, KRT86, CD7, IGLC3, TBX21, GNLY, TRDC, CD160, PYHIN1, IGLV4-60, SERPINA9, CD28, RP4-539M6.22, PGLYRP2, CR2, IL22, SLAMF6, CD8A, P2RX5, IGHG1, MS4A1, RP11- 305L7.3, IGHG4, SIT1, KLRD1, CD70, IGLC7, RASGRP1, CD96, TNFRSF13B, TMIGD2, AC096579.13, CLEC2D, CTLA4, IFNG-AS1, RP11-455F5.5, ATG9B, POU2AF1, ABCD2, RGL4, UBASH3A, CARD11, IGKC, AC104024.1, CD8B, IGHD, CD19, PAX5, SCML4, CTC-378H22.1, GATA3, RP11-279F6.3, TCL1A, TRGC1, IGHA2, KLRC2, PTPRCAP, AGAP2, FCRL6, ICOS, CD27, BLK, CXCR6, SLA2, WNT10A, CDK5R1, FCRLA, BCL11B, AL928768.3, MZB1, NELL2, GPR171, IL2RB, KLRC1, PCED1B, TRAC, DERL3, FCRL5, TSHR, RP11-284N8.3, TBC1D10C, VPREB3, GPR18, PRF1, PCED1B-AS1, RP11-290F5.1, MIXL1, AC006129.2, AC096579.7, SAMD3, PDCD1, IL18RAP, AC017104.6, CPA5, SH2D2A, ACAP1, ZNF831, RP11- 861A13.4, IGKV6D-21, WT1-AS, SEPT1, FAIM3, IGLL1, BFSP2, IKZF3, IGLV6-57, BCAS4, KCNA3, TNFRSF13C, GZMB, IL23R, CNR2, LAIR2, IGLV2-11, SLFN12L, TPRG1, STAT4, BACH2, PKHD1L1, SPOCK2, RP3-455J7.4, ZBED2, DENND2D, RP11-693J15.5, RP11-316P17.2, RP11-493L12.4, LINC00426, TNFRSF17, TNFSF8, CRTAM, LINC00525, IL7R, FCER2, RORA, STK17A, NKG7, ANKRD44-IT1, CPNE7, RP11-18H21.1, RIC3, LY9, RP11-492E3.2, SLAMF1, CCR4, TNFRSF18, IGJ, RP11-489E7.4, NLRP7, CD79A, RP11-382J12.1, LAG3, HOPX, TNFSF14, RP11-542M13.3, P2RX5-TAX1BP3, FGF23, SUSD4, CD79B, RP11- 94L15.2, PIM2, SELL, FAM129C, RP11-539L10.2, SEPT6, EVL, SP140, LINC00649, AP001046.5, P2RY11, TMC8, AC069363.1, MYL2, BZRAP1-AS1, TTC39C, PPP2R2B, SPINK2, SYNGR3, RP3-370M22.8, NCR3, RP11-117D22.2, CD5, TAGAP, ICAM3, RP11-413H22.2, FAM46C, LTB, IKZF2, TMEM156, RAPGEF6, PPP2R5C, OXNAD1, MYBL1, ITGAL, FAM65B, PHTF2, PRKCQ-AS1, BIN2, XKR6 M.CD69neg_Mast ASIC3, AD000671.6, SIGLEC8, ITGA2B, AMHR2, TSTD3, CYP51A1, EXD3, CDK15, ABCB8, SLC4A2, NSMCE1, FAM212A, KRT1, RSAD2, IL9R, WBP1, NCOA4, MAML1, MS4A2, GPR35, GALNT6, UBA7, ARHGEF6, CAPG, GRAP2, AJ271736.10, IGFLR1, PAQR5 M.CD69pos_Mast CTC-537E7.3, LINC00323, IL1RAPL1, C19orf81, ATP1A4, PTGER3, ENPP3, IL5RA, RP11-16E12.1, CMA1, AC020571.3, PPM1H, AC004510.3, PPP1R15A, RAB27B, MIR3188, GPR65, RP4-794H19.2, ALAS1, RP11- 422J8.1, ST8SIA6 M.Cycling RP11-6F2.5, HSF2BP, RP11-798K3.3, ZNF565, RP11-190C22.8, RP11-212I21.4, RNASE2, COQ2, RP11- 792D21.2, IQGAP3, ZNF724P, RP13-270P17.1, TIMM21, E2F7, C20orf201 M.DCs RP11-404O13.5, RP11-863P13.4, SLAMF9, CTD-2006K23.1, CLEC4F, CYSLTR2, CD207, RUFY4, CTD- 2319I12.1, CD1E, RP11-379F4.9, RN7SL472P, CD1C, RP11-863P13.3, CLEC10A, FLT3, RP11-24F11.2, RP3- 399L15.3, CLEC9A, RYR1, AP003774.6, AC144521.1, SIRPB1, CD1B, PPM1J, RN7SL698P, HCAR3, CD80, HCAR2, RP11-192H23.8 M.Macrophages AC005082.12, ACSM5, NT5DC4, RP11-426L16.8, RP11-452C13.1, RP11-489O18.1, RP11-760N9.1, PLA2G2D, CCL24, CCL18, MERTK, FABP3, MSR1, SIGLEC1, TMEM86A, CTB-138E5.1, CTD-2337J16.1, NPL, ATOX1, FOLR2, ACP5, NR1H3, DNAJC5B, TCHH M.Mast AMHR2, CDK15, CTC-537E7.3, GCSAML, RP11-501J20.5, TACR1, XXbac-BPG13B8.10, LINC00323, AC004791.2, MS4A2, TPSD1, GATA1, IL1RAPL1, CALB2, RP11-354E11.2, TPSAB1, SLC45A3, C1orf186, CMA1, HDC, SVOPL, CTSG, CTD-3203P2.2, MAOB, KRT1, CPA3, IL13, LTC4S, GATA2, SLC18A2, ATP1A4, DKFZP434E1119, ADCYAP1, VWA5A, SIGLEC8, LEO1, ITGA2B, NTRK1, UTS2, EFHC2, AJ271736.10, RAB27B, RP11-557H15.4, SMYD3, STXBP6, ADRB2, IL9R, HS3ST1, ATP6V0A2, AC020571.3, SAMSN1, P2RX1, GMPR, IL5RA, TIAM2, PLIN2, CTNNBL1, TDRD3, MITF, PIK3R6, MAML1, PPM1H, ACOT7, NSMCE1, ST8SIA6, CATSPER1, CRBN, RP11-620J15.3, SMIM1, GLUL, PPP1R15A, NDST2, CAPG, BMP2K, FAIM, GPR65, ALAS1, RP11-422J8.1 M.Monocytes ACSM5, AP003774.6, AQP9, C19orf59, CD1B, CD300E, CD300LB, CEACAM4, CLEC4D, CLEC4F, CLEC5A, CLEC9A, CRHBP, CTB-138E5.1, CTD-2337J16.1, EMR3, FCGR1A, FCGR1B, FPR2, HK3, IL22RA2, IL27, KCNK13, LILRA1, LILRA3, LILRA5, LILRA6, MARCO, MEFV, MRC1, MS4A14, NT5DC4, PKD2L1, RETN, RN7SL138P, RNASE2, RP11-365O16.3, RP11-404O13.5, RP11-472N13.3, RP11-489O18.1, RP11-556E13.1, RP11-737O24.5, RP11-760N9.1, RP11-798K3.3, RP5-899E9.1, S100A12, SIGLEC1, SLAMF9, SUCNR1, TCHH, TIFAB, TREM2, VSTM1, ZDHHC19, FCN1, CD1E, LILRB2, CD207, CLEC4E, SDS, C1QA, C1QC, CSF1R, CD209, MS4A6A, C1QB, MSR1, CLEC10A, S100A8, PLA2G7, IGSF6, ATP6V0D2, RP11-190C22.9, CCL18, CSTA, FPR3, CD163, DNASE1L3, FPR1, MMP12, AIF1, CACNA2D3, CSF2RA, OLR1, VSIG4, F13A1, LILRB5, IL1B, P2RY13, NCF2, LILRB4, GSDMA, RP11-290F20.3, CSF3R, PLA2G2D, MS4A4A, DLEU7, RP11-1143G9.4, LYZ, S100A9, PILRA, MRC1L1, SLAMF8, OSCAR, FCGR2A, HCAR3, CFP, LILRB3, CPVL, CLEC4A, RP11-6F2.5, FLT3, MS4A7, C5AR1, KB-1507C5.4, VMO1, MPEG1, MNDA, FOLR2, GPR84, RP11-426C22.5, RAB42, IL1RN, FUCA1, IFI30, SIGLEC12, G0S2, RP3-460G2.2, MMP9, FTL, RNU5B-1, NLRP3, AURKC, TREM1, SIGLEC15, CLEC7A, TLR2, CD14, SLC7A7, CD68, MERTK, ACP5, NLRC4, RNASE6, TLR4, RP11-792D21.2, CD163L1, TFEC, RRAGD, FAM26F, CTSS, TLR8, ATP6V1B2, STAB1, GPX1, NFAM1, LIP A, TTYH3, SAT1, APOC1, CMKLR1, THEMIS2, ATF5, CTD- 2319I12.1, LGMN, SPI1, FABP3, CTSB, CTD-2319I12.2, TNFAIP8L2, CLEC4G, CTD-2006K23.1, NAIP, CTC- 205M6.5, TNNI2, OTOA, CST3, MYCL, SLCO2B1, CCL3L1, RB1, HLA-DPB1, RGS18, GRN, HLA-DPA1, EREG, P2RY6, PLAUR, CD1A, SLC31A2, CXCL3, LILRA2, CARD9, NAGA, TYMP, FZD2, GM2A, TRPM2, NUP214 M.Myeloid AC004791.2, AC011899.9, ADCYAP1, AMHR2, AQP9, C19orf59, CD1B, CD300E, CD300LB, CDK15, CEACAM4, CLEC4D, CLEC4F, CLEC5A, CLEC9A, CMA1, CRHBP, CTB-138E5.1, CTD-2337J16.1, EMR3, FCGR1A, FCGR1B, FPR2, GATA1, GCSAML, GPR141, HK3, IL22RA2, IL27, KCNK13, LILRA1, LILRA3, LILRA5, LILRA6, MARCO, MEFV, MS4A14, MS4A2, PKD2L1, RETN, RN7SL138P, RNASE2, RP11- 354E11.2, RP11-365O16.3, RP11-472N13.3, RP11-489O18.1, RP11-501J20.5, RP11-556E13.1, RP11-760N9.1, RP11-798K3.3, RP5-899E9.1, S100A12, SIGLEC1, SIGLEC8, SUCNR1, TCHH, TIFAB, TREM2, XXbac- BPG13B8.10, FCN1, CD1E, LILRB2, HDC, CTSG, CPA3, CD207, SLC18A2, CLEC4E, SDS, C1QA, C1QC, CSF1R, MS4A6A, CD209, FCER1A, C1QB, MSR1, MMP12, CLEC10A, S100A8, LINC00323, IL1B, PLA2G7, IGSF6, ATP6V0D2, RP11-190C22.9, MS4A4A, CCL18, FPR3, AIF1, CD163, DNASE1L3, FPR1, SIGLEC12, SVOPL, CSTA, CACNA2D3, TPSD1, CSF2RA, OLR1, ATP1A4, VSIG4, ADORA3, F13A1, LILRA2, TPSAB1, LILRB5, IL1RAPL1, NCF2, P2RY13, KRT1, RP11-290F20.3, CSF3R, LILRB4, DLEU7, CALB2, S100A9, SLC45A3, GSDMA, LYZ, PLA2G2D, NLRP3, PILRA, RP11-1143G9.4, C1orf186, MRC1L1, UTS2, HCAR3, FCGR2A, SLAMF8, CFP, LILRB3, OSCAR, CTD-3203P2.2, CPVL, CLEC4A, FTL, MAOB, C5AR1, IL13, MS4A7, GPR84, VMO1, CD68, MNDA, RENBP, IL1RN, MPEG1, RP11-426C22.5, RAB42, FLT3, FOLR2, IL10RB-AS1, LTC4S, G0S2, DKFZP434E1119, FUCA1, IFI30, RP3-460G2.2, GATA2, CST6, MMP9, TREM1, ATP6V1B2, GLUL, PLIN2, VWA5A, ACP5, CLEC7A, MERTK, TLR2, AURKC, RRAGD, CD14, RP11- 792D21.2, SLC7A7, SLC11A1, CXCL16, RP11-76E17.3, RNASE6, EMILIN2, TLR4, SAT1, LEO1, GM2A, CD163L1, TLR8, GPX1, FAM26F, CTSS, TBXAS1, TNNI2, HS3ST1, ATP6V1F, NLRC4, TFEC, RNF130, CTD-2514K5.2, STAB1, TTYH3, LIPA, NFAM1, ITGA2B, MPP1, RASGRP4 M.Neutrophils AQP9, C19orf59, S100A8, MARCO, S100A12, FPR2, CD300E, VSTM1, S100A9, APOBEC3A, RP11-290F20.3, RETN, IL1RN, SLC11A1, LILRA3, FCN1, RP11-701P16.5, G0S2, RP4-613B23.1, EREG, NLRP3, RP11- 598F7.3, CXCL10, NUP214, FPR1, C5AR1, LUCAT1, TREM1, PLAUR, RP11-47I22.2, CLEC4D, LILRA5, SOD2, KYNU, TLR2, ACSL1, CLEC4E, LILRB2, KB-1507C5.4, STXBP2, CSF3R, CDC42EP2, P2RY2, STX11, OLR1, IL10RB-AS1, CEACAM4, OSM, TYMP, SLC43A2 M.Tissue_DCs RP11-404O13.5, RP11-863P13.4, SLAMF9, CTD-2006K23.1, CLEC4F, CYSLTR2, CD207, RUFY4, CD1E, RP11-379F4.9, CD1C, RP11-863P13.3, CLEC10A, RP11-24F11.2, RP1-90J20.12, RP3-399L15.3, RYR1, AP003774.6, CTB-113P19.5, SIRPB1, AC144521.1, CD1B, HCAR3, HCAR2, RP11-192H23.8, RP11-737O24.5, UTF1 M.Tolerogenic_DCs GPR157, PTGES3L, RP3-508I15.22, CTD-2319I12.1, FBXO27, BATF3, CLEC9A, DGAT2, PPM1J, IDO1, AC120194.1, TNNI2, TOMM34, SERPINF2, CPVL, SLAMF7, DICER1-AS1, C1orf54, WDFY4, CPNE3, MREG, CD3EAP, KIAA0226L, VAC14, LGALS2, PPT1, CAMK2D, SNX3 T.Activated_CD4_hiFos CYP2E1 T.CD4 CCDC81, LINC00880, CCR4, GNG8, FOXP3, F5, RN7SL443P, RP11-265P11.2, ITPKB-AS1, AC013264.2, CDKL2 T.CD8 KIR2DL4, RP11-713M15.1, TMEM155, AC131056.3, ADRB1, RP11-535A5.1, TRGC2, TPRG1, CD8B, CACNA1C-AS2, CCL4L1 T.CD8_IELs KIR2DL4, RP11-713M15.1, ADRB1, MUCL1, DPH1, KLRC2, DRAXIN, RP11-535A5.1, TRGC1, TRGC2, FBXO2, RP11-446N19.1 T.CD8_LP TMEM155, AC131056.3, CCL4L1, TRAV38-2DV8, GZMK T.CXCR6_Th17 TRAV17, BTBD16, TMPRSS3, IL17A, INSL3, MATN1-AS1, CA10, CTD-2007H13.3, KLRB1, SMG8, NMRK1, IL17F, AC092580.4, ADAM12 T.Cycling_T PKHD1, RP11-631N16.2, PRIM1, ASPM, CDCA4, AC010761.8, AC109333.10, CENPF T.ILCs LINC00299, SPINK2, RP4-673M15.1, LEKR1, CSF2, ALDOC, RUNX2, IL4I1, RP11-977G19.12, PRAM1, FXYD7, KRT86, COL9A2, LTB4R, ETV3, RP1-102K2.8, BEX2, ARL5B, CASP3, PRMT10, KRT81, CAT, TLR1, LDLRAD4 T.MT SMC5-AS1, PAQR3, PDE7A, EPHA1-AS1, RP11-277L2.4, ZNF740, BCL11B, LINC00680, ANKRD44, ZNF736, CTB-31N19.3, LSM11 T.NK KLRF1, GPR97, KIR3DX1, TEX22, CLIC3, KLRC1, S1PR5, SH2D1B, BCO2, C21orf67, SCXA, XCL2, PRF1, GZMB, ZNF114, IL2RB, CTSW, ZNF852, FCGR3A T.PD1_CD4 IL4, RP11-148O21.6, PHEX, RP11-279F6.3, CXCL13, RP11-431M7.3, TSHR, RP5-1028K7.2, ECEL1, BTLA, AC011893.3, CXXC11, SARDH, RP11-219B17.1, CD200, AC006129.4, SCGB3A1, BZRAP1-AS1, RP11- 455F5.5, FKBP5, PDCD1, TMEM232, ANKRD55, TOX, PVALB, XXYLT1-AS2, AP006621.5, MYO7A, NMB, PVRIG, THADA, GAREML, GNG4, NFATC1, KSR2, IL21, PVT1, RNF19A, SYNJ1 T.Tcells AC002331.1, AC006369.2, CA10, CXXC11, ECEL1, F5, FOXP3, IL17F, IL2, IL26, PAGE5, RP11-104L21.3, RP11-265P11.2, TMEM155, TRAV13-2, TRAV36DV7, TRAV4, TRBV28, CHRM3-AS2, IL17A, RP11- 664D1.1, THEMIS, LINC00402, AC131056.3, C15orf53, RP11-291B21.2, RP4-539M6.22, CTLA4, CD8B, NELL2, CD3G, AC013264.2, CD6, CD3D, PDCD1, CPA5, LINC00243, BCL11B, BHLHE40-AS1, SUSD4, RP11-18H21.1, GNG8, LAG3, C12orf79, ABCD2, LINC00649, TRAT1, CD8A, CTC-505O3.3, CD5, HAR1B, CXCR6, CD3E, SLFN12L, PBX4, TRAC, RN7SL443P, SIRPG, GPR171, TRBC2, RP11-85K15.2, C4orf26, RP13-977J11.2, MORN3, BATF, CD28, C14orf64, AC104820.2 T.Tregs AHSP, PNMA3, SLC8A1-AS1, CARD17, FOXP3, TTBK1, RP4-533D7.5, F5, TNFRSF8, FANK1, RTKN2, IL2RA, CTLA4, CUL9, PPP1R3F, LAIR2, NINJ2, CTD-2325P2.4, BATF, TNFRSF9, AC017002.1, TNFRSF4

TABLE 7 Stromal Healthy specific markers for indicated cell types F.Crypt CFD, ADAMDEC1, MFAP4, CCL13, CCL11, HAPLN1, PTGDS, SFTA1P, CXCL1, ABCA6, ELANE, CP, CCL7, NR2F1-AS1, CXCL6, SLIT3, FZD1, CCL19, CFHR3, ADAMTS2, EPHA7, RBFOX1, RP11-93L9.1, GPC3, PTGFR, ABCA10, HAS2, SLCO1C1, FZD10-AS1, RNF112, COL6A5, RP11-222A11.1, AL132709.5, SORCS2, LCE2A, FGF10, RP11-135D11.2, CHODL, RP11-1008C21.2, GALNT9, TWIST2, AC092652.1, TNN, RP11-572C15.6 F.Crypt_RSPO3 CFH, CXCL12, CCL11, EFEMP1, ADH1B, CCDC80, C7, DPT, RSPO3, ASPN, SERPINE2, ANGPTL1, CXCL6, CP, GPC6, CHODL, CCL19, SLIT3, APOD, OGN, GREM2, MAPKAP1, PTGER1, PDE5A, GPC3, RP11- 135D11.2, RGMA, C1QTNF3, OSR2, FAIM2, PTGFR, MFAP5, BDKRB1, CAPN6, ECM2, DACT1, SHISA3, CDO1, SFRP2, SFRP4, PI16, RBBP9, FLRT2, CTD-2014B16.3, IL17RD, AL035610.1, APCDD1L-AS1, FOLH1, SORCS2, ENTPD1-AS1, GPC2, AP001626.2, CTD-2085J24.4, CTD-2083E4.4, RP4-545C24.1 F.Crypt_hiFos CNTN1, ZIC1, TMEM232, AC005592.2, ZDHHC11, SHBG, CECR5-AS1, WASF1, RNU6-450P F.Crypt_loFos_1 RN7SL374P, BVES, KCNS2, MRAP, RP11-98I9.4 F.Crypt_loFos_2 ZNF836, FAM102B F.Endothelial AC004540.4, AC116035.1, APLN, AVPR2, CCDC178, CNTNAP3B, COX4I2, FAM155A, FCN3, FOXC1, GABRD, GIPC3, GJA4, GPIHBP1, INHBB, KCNJ8, KRT222, KRT27, LCN6, LYVE1, NOVA2, NPR1, PGM5- AS1, PLA1A, RASSF9, ROPN1L, RP11-1024P17.1, RP11-536018.1, SCN3B, SELE, SELP, SNTG2, SOX18, STC1, STC2, TLL1, TSPAN18, KDR, FAM110D, TM4SF18, H19, DARC, MMRN2, C1QTNF9, RAMP3, ZNF833P, FAM167B, PLVAP, BCL6B, AC011526.1, CLDN5, MYCT1, HIGD1B, SHANK3, CXorD6, FLT1, ECSCR, RP11-251M1.1, SLC14A1, ROBO4, VWF, RP11-536O18.2, CYYR1, CDH5, TMEM88, ZNF385D, GPR116, THSD7A, ESAM, APLNR, USHBP1, SOX17, ADM5, SNCG, CD320, RAMP2, ARHGEF15, CD34, CALCRL, EGFL7, GALNT15, NOS3, MADCAM1, FLT4, ANGPT2, ELTD1, THSD1, PODXL, KANK3, GPRC5B, ARAP3, SERPINE1, TNNT1, CYP1B1-AS1, KIAA1462, RP11-23P13.7, TPO, TEK, JAM2, VEGFC, HYAL1, CKMT2, RAPGEF3, MKL2, PALMD, RGS5, CLEC14A, CCL14, NOTCH3, PTPRB, NOSTRIN, LRRC46, PCDH12, TSPAN7, GPR4, EXOC3L2, SEMA6C, RUNDC3B, S1PR1, CD36, TDRD10, FABP5, ERG, NOTCH4, GRB10, GPR1, EHD4, MAPK11, EXOC3L1, RASIP1, SEMA3F, IGFBP4, PKN3, BTNL9, HSPA12B, RND1, GNG11, ZNF541, FGD5, NUAK1, PKP4, HYAL2, ACE, EVA1C, RP11-473M20.9, SLC35G2, HRC, IPO11, SLC9A3R2, ENPP2, SHE, ARC, MPZL2, ZNF676, RBP7, EPM2A, JAG2, RP11-768F21.1, CD93, SEMA3G, SLC7A2, LINC01013, EPAS1, MASP1, ASB9, ADCY4, MYRIP, RP11-435O5.5, LINC00162, AIF1L, DOCK9, KIF19, SPTBN5, DYSF, CYPIBI, OAZ3, FAM189A2, ENG, PRX, STXBP1, CORT, RAPGEF4, CLIC2, MEOX1, PRSS23, SOX7, SMAD1, CFI, APBB2, ARHGAP29, SH3BP5, FAM84B, ADAM15, TEAD4, CYP26B1, SERPINI1, TGFBR2, HLX, SLC25A25, AC009336.24, MIER2, TIE1, CDC37, ICAM2, CRIP2, CBX2, FILIP1, STOM, EBF1, FZD4, TNFAIP1, EPB41L4A, RIN1, IL33, TMEM255B, HTR2B, BAALC, TACC1, PLLP, CABP1, RP11-830F9.6, PTPN14, RPGR, SLCO2A1, FAM107A, APOLD1, CCDC85B, ALPL, MANSC1, ITGA5, EPHB4, MFAP3, EMCN, MYBBPIA, FAM213A, DOCK4, CX3CL1, PLXND1, CELSR1, SHROOM4, RBP5, TINAGL1, LDB2, C10orf10, RASAL2, TMTC1, ARL15, DGKE, RP11-806H10.4, CSGALNACT1, ACVRL1, C16orf80, BCAM, PDE1C, VAMP5, TNFRSF10D, SLC16A14, MSMP, NES, KLHDC8B F.Endothelial_1 GAS1, RP11-15A1.7, SEMA3G, FCN3, STC1, MASP1, RP11-671J11.4, RP11-105C19.1, ALPL, PRDM16, ARL15, ANO2, BTNL9, RP11-435O5.5, RP11-806H10.4, AC007292.3, EFNB2, C10orf10, RBP7, SOX17, RUNDC3B, C22orf26, MECOM, RTN4R, NOV, HEY1, LCN6, TBC1D13, SSUH2 F.Fibroblast CFD, FBLN1, PROCR, BMP4, ADAMDEC1, CXCL12, DMKN, CCL8, PLAC9, SPON2, HAAO, CCL13, ADH1B, SCARA5, HAPLN1, PTGDS, CCL11, NSG1, GLT8D2, F3, GADD45G, TMEM119, LRP1, ENHO, VCAM1, FAM150B, VSTM2A, PDGFRA, AGT, SFTA1P, DPT, LOXL1, PDGFD, CXCL1, APOD, PCDH18, FARP1, PRR16, CRISPLD2, TPBG, PXDN, MXRA5, FGF7, CDH11, HTRA3, BAMBI, PLAGL1, TSLP, TDO2, GPC6, TRPA1, FGFR1, ELANE, TNC, LRRN4CL, CP, GLP2R, HSD11B1, LANCL2, SVEP1, NMNAT3, CXCL6, CCL7, REEP2, COL4A5, CIB2, WNT5B, SCUBE2, ALDH1A3, RP11-112H10.4, FZD1, FAM65C, CCL19, PCSK6, LTBP2, C3, SRPX2, FGF9, RP11-1260E13.4, NPY, DACT1, SEMA3E, GPC3, COL4A6, RP11- 449D8.1, OBSCN, RP11-93L9.1, SPOCK1, BICC1, BMPER, AC003090.1, RP11-367J11.3, PTGFR, FZD10- AS1, CRABP2, C1QTNF7, WNT5A, LOXL4, FAM19A1, RNF112, C22orf31, HMGCLL1, SAMD14, PDGFRL, AC002511.2, RP11-2E17.1, C3orf55, ATP6V1G2, COL6A5, CLSTN2, PAPLN, FOXL1, KRTDAP, C1QL1, CTB-92J24.3, LRRC15, ADAMTSL3, CTD-2314B22.3, CHODL, RN7SL336P, LCE2A, LRRC18, HS3ST3A1, GSG1L, PGR, RP11-473E2.4, ETNK2, CHI3L1, KIF7, RP11-222A11.1, AC104654.2, OGN, EDAR, MC1R, AMPH, FGF10, RBMS3-AS3, CNNM1, ZNF334, RSPO2, RP11-1008C21.2, AC004538.3, EFCAB1, GALNT9, GS1-18A18.1, RP4-755D9.1, SORCS2, RP11-135D11.2, ADCY2, LPAR3, LRRC8E, RP11-157J24.2 F.Glia ANGPTL7, CAP2, CDH19, CTD-2325P2.4, CYP27C1, DLX1, DYNC1I1, FAM181B, FGF1, FOXD3, HAND2, LINC00982, LRRC4C, LRRTM1, MGAT4C, NDP, NKAIN3, NRXN3, PCSK2, PMP2, PTPRZ1, RASGEF1C, RORB, RP11-21A7A.4, RP11-713P17.3, RP4-792G4.2, SERPINA5, SHC4, SOX10, SOX2, SRCIN1, STEAP1B, TENM3, TMEM155, VGLL3, CADM2, L1CAM, MYOT, SBSPON, TFAP2A, LINC00632, NRXN1, COL28A1, HPR, TTYH1, TMEM178A, GPM6B, PLP1, SCN7A, MPZ, CMTM5, XKR4, HAND2-AS1, C10orf82, CRYAB, SPP1, TUBB2B, LRAT, NTM, SORCS1, DLX2, NLGN4X, TMEM132B, TSPAN11, BAI3, S100A1, SOX8, ST6GALNAC2, NIM1, AC144449.1, NGFR, KCNMB4, FLRT3, RP11-166D19.1, COL8A1, AATK, SEMA3B, TMOD2, WISP2, KCTD1, TMEM59L, CAPS, CAB39L, COL9A3, SH3BGR, SCN9A, ART3, WDR86, RP11- 20J15.3, MMP17, S100B, PRIMA1, GRIK3, MAB21L1, MFAP3L, ALDH1A1, COL21A1, LEPREL1, LINC00882, SNCA, AP001631.9, GPR155, ENTPD2, CPEB1, PRNP, RFTN2, ZNF853, C1orf198, RP11- 235E17.4, CNP, RP11-187C18.2, MFSD2A, FST, OLFML2A, ASPA, ABL2, CADM4, SLC16A4, BEX1, CHADL, RCAN1, GFRA3, PCBP4, FXYD1, LGI4, ARHGEF26, CYR61, FGFBP2, EHBP1, RASSF4, COMT, TUBB4A, SECISBP2L, ITPR1, PMP22, SCCPDH, ANK3, SLC22A17, SLC16A8, NCAM1, UCHL1, ARHGAP15, FIBIN, ASTN2, MAL, AP1S2, ENDOD1, POU3F1, GRAMD3, FEZ1, SMIM5, ATL1, SEMA3C, AK5, GFRA1, SREBF1, IL11RA, KDSR, PMEPA1, FBLN2, LINC00894, RBM43, NUP188, NXPH3, ADK, CADM3, USP6, RP4-777D9.2, MATN2, C1orf204, TUBA1A, PDK4, CYP27A1, TPCN2, LAMP5, FADS3, PON2, LINC00263, ANXA2, DKK3, TTLL4, CD9, NDRG2, RTDR1, PEBP1, PAQR6, CNN3, MAPRE2, CLU, SLC15A3, LMBRD2, DEPDC7, MIIP, SPARC, SIPA1L2, ZFYVE1, TIMP3, C8orf4, GNG2, ARHGAP12, ITGB1BP1, NPTX2, CXXC5, PLSCR4, SORBS2, GATM, CRTAC1, TSPAN15, HSPA2, ALCAM, CDC42EP4, TPT1-AS1, ZBTB5, CBR1, RHOB, STARD13, SLC39A6, PLA2G16, PDLIM4 F.Inflammatory CHI3L1, MMP3, SIRT4, GBP1, TRAFD1, ZCCHC4, BLOC1S5, CDC23, VTA1, PLAU, PSME3, PAQR5, GSTT1, APOL2, CAMKK2, COMMD2, BYSL, UBIAD1, STX5, BCDIN3D, RRP1 F.Microvascular GABRD, STC2, SPTBN5, F2RL3, PASK, RP11-536O18.2, APLN, MSMP, C11orf95, IVNS1ABP, LYPD5, GIPC3, ME3, PRX, RP11-575F12.1, VWA1, RGCC, PRSS23, SEMA3F, MCPH1, ADARB1, SETD4, AC112693.2, RNF44, PGS1, EXOC3L2, BAALC, TBC1D8, DYSF, NRP1, CIT, TP53I11, WWTR1, NUP43, MICALL1, HSPG2, TBCD, HTRA1, RAPGEF4, ANRD65, SCARB1, RARG, ITGA6, ARHGAP23, JAM3, EGLN3 F.Myofibroblasts SOGA2, SOSTDC1, HSD17B6, DES, ACTG2, NPNT, AF131217.1, RP11-611D20.2, RAB9B, LUZP2, CNN1, MYLK, TAGLN, RP13-143G15.4, MYH11, SYT10, SNCAIP, LMOD1, DIO2, TMEM158, LINC00595, RP11- 356C4.3, HHIP, PDLIM3, C20orf166-AS1, SLC2A4, FBXL22, TGM2, ACTA2, LRRC17, FHL1, SLMAP, NEXN, PDLIM7, LRFN3, BVES-AS1, NAA60, TPM2, SPAG8, LPP, MIR145, KCNMB1, SMTN, MACROD2, SPESP1, TGFB1I1, AOC3, FAT4, DSTN, FLNA, RP11-344E13.3, NDUFA4, TCEAL4, MIR143HG, TRPC6, HMG20B, TES, TTLL7, SLC12A8, PDIA5, LTBP1, TCEAL1, WRN, AKAP6, PLN, SVIL, RP11-196G18.23, VAT1L, TCEAL3, TPM1, TEAD3 F.Pcap_Venules FOXC1, LYVE1, RASSF9, SCN3B, SELE, TLL1, DARC, MADCAM1, SELP, VEGFC, CCL14, LRRC46, FAM155A, ZNF385D, RAB3C, CELSR1, UBD, LINC01013, C2CD4B, ACKR4, PLA1A, TSPAN18, FAM189A2, RP13-395E19.3, GALNT15, RP5-1021I20.5, CITED4, DUSP23, GPR126, TIAM1, CPE, DTL, ZSCAN31, ICAM1, AMDHD1, ICAM4, KCNMB3, CORT, HTR2B, PMEL, CYP1B1, KLHL3, HESX1, LPCAT4, ZNF521, APLNR, KIAA1683, NR5A2, PRKAR1B, FAM84B, MEOX1, IFIH1, SEMA6A F.Pericytes EDNRA, CYP4X1, KCNJ8, COX4I2, STEAP4, RP11-714L20.1, GJC1, CCDC3, HRC, NOTCH3, FAM162B, CDC7, RGS5, ITGA7, PRDM11, BGN, HIGD1B, LDB3, JRKL, NR2F2-AS1, NDUFA4L2, NR1H4, PDGFRB, PGF, ATXN7L2, LINC00883, TEPP, ARHGEF17, UBA2, REM1, ISYNA1, FZD7, TNS1, PLXDC1, CSRP2, OLFM2, GJA4, TMEM38A, NUP133, SERPINI1, TINAGL1, RNF208, EBF1, HES4, SUSD2, CNNM2, ADAMTS1, ATP1B2, EPS8, MCAM, RP11-110I1.12, RP11-349A22.5, ADIRF, TPPP3 F.Stromal CXCL14, A2M, CALD1, C1S, MFAP4, COL6A2, COL3A1, PLAT, CFD, DCN, TM4SF1, CYGB, TCF21, LUM, FBLN1, SOD3, ADAMDEC1, MMP2, PROCR, COL6A1, BMP4, CXCL12, TPM2, FABP5, MFGE8, CLEC11A, EPHX1, CFH, CTSK, SLC9A3R2, PTN, PPAP2B, SDC2, PCOLCE, CAV1, EMILIN1, DMKN, CCL8, STMN2, LINC01082, POSTN, HAAO, FRZB, FOXF1, ADH1B, PLAU, CCL13, WFDC1, SNAI2, GGT5, PTGDS, SCARA5, CCL11, HAPLN1, ACTA2, EFEMP1, FXYD6, GLT8D2, PITX1, CAV2, FENDRR, RBP5, NKX2-3, NDUFA4L2, EHD2, CTC-276P9.1, RAMP2, CD320, NSG1, MGP, TFPI, THY1, CLEC14A, F3, FILIP1L, TMEM119, FABP4, EDIL3, TMEM204, EMID1, LHFP, TMEM100, VCAN, RCAN2, ENHO, IL34, PLVAP, BMP5, AGT, SFTA1P, FAM150B, COL6A3, LOXL1, VSTM2A, TAGLN, IGFBP5, CCDC80, PDLIM3, CLDN5, CERCAM, PTCH1, FN1, DPT, PDGFD, PDGFRA, MYLK, FGF7, EGFL7, RAMP3, CRISPLD2, PCDH18, TNXB, NEGR1, TAC3, GSTM5, SEPT4, PXDN, PGF, VWF, ESAM, OLFML1, MMP11, TUSC3, ECSCR, VASN, DDR2, SMYD4, EMCN, PRR16, COLEC11, MXRA5, TMEM150C, TMEM88, LRRC32, AC011526.1, C16orf89, FGFR1, VSTM4, RP11-332H18.4, NEXN, PDGFRB, NID1, FOXF2, FAM167B, COLEC12, CYYR1, HTRA3, EVA1A, ADAMTS1, SNCG, CD34, ELANE, FBN1, TDO2, MMP1, CDH11, TRIL, ELTD1, PODXL, PAMR1, RP11-532F6.3, HHIP, RUNX1T1, TRPA1, TBX2, GPC6, TEAD2, TSLP, LAMA5, RP4-665J23.1, LRRN4CL, RP11-514D23.3, HOXA11, AKAP12, TM4SF18, ARHGAP29, NR2F1- AS1, SGCA, RPS6KA2, MIR497HG, MAB21L2, HHIP-AS1, PRKG1, PLEKHH2, NTF3, PDE1A, RASIP1, GPR124, CCL7, APLNR, C7, ACTG2, CCDC102B, EFCC1, EFHD1, CP, LIFR, FAM107A, HOXD11, TFPI2, FLT1, CXCL6, SVEP1, CDH5, CH25H, HOXD8, LOX, MMRN2, SLC14A1, HSPB6, PTGES, MAPK10, ANGPT2, PTGDR2, SPON1, GLP2R, NKD2, LAMC3, CLMP, ROB04, SLIT3, MRVI1, FAM110D, CALCRL, MYCT1, NUAK1, CXorf36, PTPRM, RHOJ, ENPP6, NR2F1, RP11-112H10.4, OSMR, KDR, RGS5, GPR63, COL12A1, COL4A5, MIR143HG, LTBP2, ARHGEF25, HOXD9, C3, DARC, WNT5B, RP11-383H13.1, NXN, SOSTDC1, GPR116, REEP2, RP3-323P13.2, AC131025.8, FZD4, GLI1, TNFRSF10D, SYNDIG1, MIR145, PCDH7, CFHR3, LPHN2, RP11-536O18.2, FGD5, GRB10, SOBP, MADCAM1, PALMD, SULF1, PCSK6, HSPA12B, ZP1, ALPL, AC124789.1, TEK, SOX17, SOX18, VAT1L, FAM162B, USHBP1, DACT1, PTPRG, PDE7B, AC156455.1, CHST1, SALL1, PEAR1, C1orf167, SEMA3E, ASPN, OSR1, CLEC3B, FNDC1, FILIP1, FAM13C, LEPR, AC116035.1, GPRC5B, PREX2, PCDH12, CCL21, CABP1, ROR2, DZIP1, HIGD1B, COL4A6, RSPO3, WDFY3-AS2, PDGFC, LCN6, AMOTL1, HYAL1, KCNE4, TMTC1, NPY, PRX, ADM5, TBXA2R, LRRC17, RBFOX1, GLIS2, SYNPO2, FAM110B, RP11-264B14.1, AP000330.8, GPR4, NTN1, EDA2R, BOC, ISL2, DHRS7C, EXOC3L2, LINC00961, RP11-449D8.1, PCDH19, C16orf46, RBPMS2, NOS3, HOXC9, SEMA3A, BCL6B, KLHL13, SEMA6C, ARHGEF15, ACSS3, HOXC6, PTGFR, WNT5A, IGF2, SPOCK1, ADAMTS4, HSD17B6, CPAMD8, HIF3A, COX4I2, FAM19A1, PPP1R3C, TEKT3, CLSTN2, NPR2, FOXL1, LINC00839, RGMA, MFAP5, PHACTR3, SLCO1C1, LCA5, AC017048.4, BICC1, ZNF423, SLC16A2, AC003090.1, ANGPT1, C1QL1, COL6A5, KRT222, NPR1, MUSK, NOTCH3, THSD1, FMO3, NDNF, SAMD14, APLN, AVPR2, PABPC5, ZNF833P, SCGB1B2P, ZNF385D, GALNT15, AC061992.2, AC002511.2, CRMP1, FAM171B, HOXC8, HMGCLL1, FBXL7, SERPINE1, C22orf31, FGF13, PDGFRL, ADAMTS5, C1QTNF7, GSG1L, KRTDAP, NAP1L3, RP11-2E17.1, ADAMTSL3, FAT4, ARHGAP28, TRPC6, CASP12, RNF112, EVC, FOLR1, CHODL, CTB-92J24.3, LINC00475, OGN, CDO1, ETNK2, PAPLN, IL33, KIF7, DIO2, GJA4, HS3ST3A1, INHBB, KIAA1462, LRRC3B, PTH1R, CORT, C3orf55, C1QTNF9, MMP3, AC116366.6, C10orf107, CHRD, NAALAD2, RP11-572C15.6, RP4-755D9.1, STC1, INMT, BHMT2, SUSD2, CTD- 2314B22.3, GLIS1, RP11-774O3.3, AGTR1, CILP, ECM2, FCN3, GRIA4, GRID1, HPSE2, LRRC18, OMG, RAET1G, RP11-54O7.3, RP11-135D11.2, SHANK3, GPR176, RP11-486G15.2, ZDHHC15, RP11-1008C21.2, CNNM1, TTLL11, CCDC178, FAM180A, LRRC15, RP11-395L14.4, SELP, SORCS2, TRPC1, H19, NUDT10, CHI3L1, TRO, MIR503HG, AC092652.1, FGF10, GPIHBP1, LCE2A, LIFR-AS1, MYL3, NOVA2, RBMS3- AS3, RNF150, RP11-710C12.1, RSPO2, GPR133, RP11-251M1.1, LINC00595, ZNF667, CACHD1, AL132709.5, PARD6G, RP11-69I8.3, FLT4, RP11-314C16.1, SLC45A1, C17orf51 F.Villus DNAI1, F2RL2, GRIN2A, GS1-18A18.1, NEFM, NOTO, RP11-157P1.4, RP11-804A23.4, RP4-755D9.1, RSPO2, REEP2, COL4A6, GLP2R, DLEU7, EDAR, SCN3A, PCSK6, SCUBE2, WNT5B, AC002511.2, RP11- 1002K11.1, HS3ST3A1, LPAR3, FGF9, LANCL2, DHRS7C, C22orf31, AC003090.1, ENHO, EGOT, BAMBI, TSLP, SCUBE1, KCNK17, BMP7, VSTM2A, FAM150B, ADAMTS13, MMP11, KREMEN1, SRPX2, RBP4, CBLN2, POSTN, CHST1, NRIP3, NSG1, OBSCN, NMNAT3, TSPAN33, CNTFR, SEMA4D, SEMA3A, FAM218A, C1QL1, EDNRB, PDGFRA, PTGIS, MFAP2, SHANK2, TSHZ2, SDK1, DDHD1, GSG1L, CTD- 2334D19.1, ZNF407, LAMC3, GADD45G, TPBG, RP11-449D8.1, WFS1, CNIH3 F.Villus_1 IP6K3, MSX2, NTRK3, TTC25, AC019171.1, MAST1, AC022007.5, ARHGEF33, EGOT, KB-1125A3.11, RP11-473M20.16, AL163953.3, XXbac-BPG252P9.10, EDAR, NHS, CASC14, ADCY2, AC009480.3, CPM, RN7SL336P, FBXW7, BDNF, CTD-3093M3.1, FGF9, HUS1B, RP11-309M23.1, C10orf107 F.Villus_2 GRIN2A, NEFM, VPS37D, F2RL2, LEF1-AS1, DHRS7C, AC096772.6, RP11-86H7.7, RP11-97O12.7, LAMTOR5-AS1, ZNF646, EFHB, RP11-144G6.12

TABLE 8 Stromal UC specific markers for indicated cell types F.Crypt AC004538.3, AL132709.8, CILP, COL6A5, FMO2, GRIK4, HHIPL1, MPP2, OMG, RN7SKP295, RP5- 1172A22.1, SHISA3, SLC17A7, TEKT3, TMEFF2, CNTN1, CCL13, GAS6-AS2, LPAR4, CCL7, OGN, AL035610.1, ABCA8, ABCA9, CP, CCL11, SVEP1, ELANE, ADAMDEC1, ANGPTL1, RP11-572C15.6, RP11- 473E2.4, GPC3, HAPLN1, CFD, SFTA1P, NAALAD2, ADH1B, CCL8, SCGB1B2P, ANKRD13B, CCDC80, FBLN1, ABCA10, ADAMTSL3, CPEB1, DNM1, APOE, PTGDS, SCARA5 F.Crypt_RSPO3 SMAD5-AS1, OGN, CCL19, CAPN6, GREM1, SFRP4, CCL21, C7, PCOLCE2, GREM2, RP11-339B21.13, RP11-195F19.9, PI16, NAALAD2, RP11-572C15.6, CHODL, RSPO3, CCDC80, MAPKAP1, RGMA, NPB, OSR2, GNB3, SFRP1, RP11-597D13.9, FLRT2, ZNF3, C1QTNF9B-AS1, CTC-559E9.6, ADAMTSL3, RNF146, SIMC1, CP, PTGDS, ANGPTL1, DPT, FMR1, SRPX, CXCL12, ADH1B, EFEMP1, COL14A1, IRF2BP1, ZNF398, CFH, COPRS F.Crypt_hiFos RP11-173B14.5, TMEFF2, BCDIN3D-AS1, LPAR4, CTD-2651B20.3, RP11-420L9.5, CPEB1 F.Crypt_loFos_1 BPI, AL132709.8, RP11-216B9.6, PNMA2 F.Crpt_loFos_2 RP11-588K22.2, RN7SKP295, PIP4K2B, MAP3K10 F.Endothelial AC116035.1, C1QTNF9, C1QTNF9B, CASC10, CTD-2536I1.1, CYP1A1, ESM1, FAM69B, GABRD, GALNT15, GJA5, GPIHBP1, GSDMC, KRT222, KRT5, LHX6, LYVE1, MMRN1, NOVA2, NOX4, PDE10A, RASSF9, RP11-286H15.1, RP11-676J12.6, STC2, ZNF541, ZNF833P, ZNF385D, LCN6, KDR, H19, HIGD1B, CXorf36, TM4SF18, AC011526.1, ECSCR, PLVAP, APLNR, SELE, FAM110D, CLDN5, DARC, RP11- 251M1.1, VWF, SNCG, FCN3, ESAM, GPR4, FAM167B, COX4I2, MADCAM1, GPR116, SOX17, SHANK3, CDH5, CLEC14A, TLL1, ARHGEF15, EXOC3L2, CORT, RP11-536O18.2, RP11-536O18.1, ROBO4, AVPR2, INHBB, GAS1, MYCT1, BCL6B, THSD1, EGFL7, RAMP2, FLT1, RAMP3, SOX7, CD34, TMEM88, SOX18, TPO, CD320, MMRN2, RP11-23P13.7, KL, FUT1, SLC14A1, RP11-159D12.10, HSPA12B, PODXL, USHBP1, ADM5, CCL14, ANGPT2, ANKRD29, ELTD1, RND1, CCDC3, JAG2, PCDH12, TNFRSF10C, TEK, KCNJ8, KIAA1462, KANK3, ADCY4, RBP7, CYYR1, FOXS1, APLN, SELP, VEGFC, GRB10, CPLX1, JAM2, BFSP1, CALCRL, NPR1, GPRC5B, BTNL9, TSPAN7, C22orf34, PALMD, RP3-473L9.4, RASIP1, IGSF9B, F2RL3, RTN4RL2, RAPGEF3, ERG, ARHGAP29, BAALC, GJA4, EMCN, DYSF, FGD5, FABP5, HYAL2, PKN3, ENG, CTD-2135D7.5, CD36, TIE1, ALPL, SFTA2, SLC9A3R2, EPAS1, RP11-355F16.1, CD93, ACE, NUAK1, TSPAN18, DOCK9, PTPRB, SNTG2, AC009336.24, LEPR, CABP1, RAPGEF4, GPR146, NOSTRIN, EVA1C, ADAMTS4, ICAM2, SEMA3F, TNFAIP1, CSGALNACT1, MIER2, CRIP2, RASA4, MPZL2, KIF26A, SMAD1, SHROOM4, CPXM2, GNG11, EXOC3L1, IFI44L, RP11-830F9.6, SERPINI1, RGS5, DGKE, SHE, LTF, NDST1, LDB2, ADAM15, OAZ3, MYBBP1A, PLA1A, FZD4, C4orf32, SLCO2A1, RP11-92C4.6, AQP1, CACNG8, DLL4, CYP1B1-AS1, TGFBR2, GIMAP8, NOTCH4, IPO11, PCDH17, KCNC4, CUBN, NDUFA4L2, MAPK11, MKL2, PLCB1, APBB2, CFI, C2CD4B, STOM, TMEM204, CASP12, FAM107A, RBP5, SEMA6C, FAM65A, HEG1, PKP4, SLC35G2, PEAR1, SCARF1, EDN1, FAM219A, ARAP3, SYNPO, RAI14, SH2D3C, S1PR1, EHD4, CCDC85B, MTUS1, FAM13C, CLEC3B, RUNDC3B, ENPP2, C11orf95, BCAM, ASB9, IGHV3-64, FKBP1A, TINAGL1, LIFR, PTRF F.Endothelial_1 FGF12, GJA5, SEMA3G, PDE10A, IGFBP7-AS1, PRODH, RP11-789C17.1, FCN3, TNMD, GPIHBP1, IGF2, SLC6A6, JAG2, ARL15, ALPL, EDN1, HEY1, AQP1, CTD-2035E11.4, RP11-225B17.2, AIF1L, SOX7, RP11- 576D8.4, ANKRD29, RBP7, SRP14 F.Fibroblast AC002511.2, AC004538.3, AKNAD1, AL132709.8, CHRM2, CILP, CLSTN2, COL6A5, CTD-2078B5.2, CTD- 2334D19.1, FAM19A1, FAM216B, FGF10, FGF14, FMO2, GLIS1, GREM1, GRIK4, HOXC8, HTR2A, KRTDAP, LIFR-AS1, LRRC15, LRRC18, NACAD, NKX3-2, NPY, OMG, PPAPDC1A, RBMS3-AS3, RN7SKP295, RP11-129B22.1, RP11-395L14.4, RP11-473E2.4, RP11-473L15.2, RP11-7O14.1, RP11-800A3.7, RP3-323P13.2, RP4-530I15.6, RP5-1172A22.1, RSPO2, SHISA3, SLC17A7, STRA6, TCEAL5, TEKT3, WISP1, DPT, SEMA3E, CCL13, CNTN1, FAM19A5, CCL11, AC104654.2, LTBP2, THBS2, ADORA1, HS3ST3A1, IL13RA2, ADAMTSL3, MMP3, VSTM2A, IL11, FAM150B, GLP2R, CHI3L1, GAS6-AS2, SCUBE1, CCL7, RP11-449D8.1, SFTAIP, COL4A5, CHODL, AL035610.1, RP11-112H10.4, DMKN, PDGFRA, RP11-588K22.2, PCOLCE2, NSG1, COL4A6, OXT, WNT5B, SVEP1, OGN, C3, REEP2, CPXM1, SYNDIG1, CYP27C1, F3, LRRN4CL, TNFRSF11B, RP11-572C15.6, SDK1, MMP1, ARL9, ENHO, LRCH2, CP, RNF150, MXRA5, SCARA5, DACT1, FAM65C, ABCA9, TMEM119, RP11-1002K11.1, CYS1, CCL19, SRRM3, COL7A1, SCUBE2, ABCA8, HTRA3, ADH1B, PCSK6, APOD, HAS1, DNM1, FGF7, VCAM1, HMGCLL1, ELANE, ADAMTS13, STMN2, BMP4, RP11-69I8.3, PRR16, RP11-152P17.2, BMP7, PIEZO2, CTSK, NPPC, AKR1C1, CTD-2269F5.1, C1QL1, C10orf107, GPC3, FIGN, LOXL1, CCDC71L, CFD, DZIP1L, RP11-204M4.2, FGF9, PI15, DHRS7C, ANGPTL1, GLT8D2, FANCC, BMP5, PROCR, ADAMDEC1, TRPA1, NAALAD2, GPR133, PTGIS, RP11-284F21.8, KB-1125A3.11, GSTM5, LOX, HAPLN1, FBLN1, LAMA2, PLAU, RARRES2, LRP1, CCDC80, PRTG, WNT2 F.Glia ADAMTS8, ANGPTL7, CADM2, CDH2, CMTM5, CRTAC1, FOXD3, L1CAM, NRXN1, PCSK2, PMP2, RP11- 189B4.6, RP4-792G4.2, SERPINA5, SOX10, TENM3, TFAP2A, CDH19, MYOT, GPR17, PLP1, SOX2, LRRTM1, MPZ, COL28A1, XKR4, PPT2-EGFL8, DLX2, PRIMA1, HAND2-AS1, STEAP1B, NTM, GPM6B, AKAP6, LINC00162, SHC4, AC004466.1, CRYAB, DYNC1I1, WISP2, MAB21L1, TMEM59L, ST6GALNAC2, KIRREL3, HAND2, KCNMB4, NRXN3, RP11-262H14.3, TGFB2, SORCS1, NXF3, CADM4, TUBB2B, NGFR, HOXC6, MFAP3L, HOXC9, S100A1, LOXL3, ART3, TTYH1, CAPS, KCTD1, SEMA3B, MMP17, MEGF6, SPP1, COL8A1, RP11-18H7.1, FSTL3, COL9A3, COL21A1, NLGN4X, PMEPA1, DHH, RP4-635E18.6, RP5- 1126H10.2, PRNP, TPT1-AS1, UBR4, GAS7, MIA, TSPAN11, GPR155, GFRA3, SLC22A17, SCN7A, SCRG1, EGFL8, TTR, NPTX2, ANKRD53, SNCA, SH3BGR, FHOD3, TIMP4, C1orf198, ITGB8, DEPDC7, GALNT2, LGI4, TSPAN15, RASSF4, TNFAIP6, SCCPDH, NUP188, OLFML2A, LAMP5, ALDH1A1, TMEM17, SEMA3C, RP5-1007M22.2, SCN9A, CNP, CAB39L, DAG1, KCNAB3, RCAN1, SLC15A3, SMIM5, CDKN2A, PMP22, BPGM, MAL, FEZ1, ARHGAP15, GDNF, RIPK4, FBLN2, CHADL, PHLDA3, S100B, SIPA1L2, CYTL1, HSPB2, DKK3, FAM210B, LEPREL1, C12orf43, IMMP2L, FAM124A, SORBS2, ITPR1, ARHGEF26, KCTD11, IER3, BMP8B, COMT, PCDH9, FST, FADS3, TXNRD2, CCL2, VPS52, PON2, CADM3, LPAR1, NRN1, ABL2, LINC00672, SREBF1, ANXA2, FRMD4A, SDC3, PDLIM4, MATN2, SLITRK6, RP11-374M1.5, RXRG, PEBP1, NLRP1, AP1S2, KCNS3, STARD13, JKAMP, GATM, CYR61, CBR1, GPC1, FXYD1, HES1, PCID2, PEPD, ADK, UPB1, CNPY2, MARCH2, S100A3, AP000688.8, B4GALT6, SPARC F.Inflammatory C22orf15, IL24, SBSN, TMEM215, TRPC4, ZNF295-AS1, TNFRSF11B, IL13RA2, CHRM2, MMP3, PI15, WNT2, CHI3L1, RP1-90J20.8, MMP10, LBP, RP4-530I15.6, STRA6, GALNT16, WISP1, TWIST2, RASL11B, PLAU, STK32B, PTGES, PPAPDC1A, TFPI2, STEAP1, BDNF, MMP1, CXCL6, HGF, RP11-204M4.2, SORCS2, GAL, LINC00944, KIAA1199, PTHLH, PPIL1 F.Microvascular SCHIP1, MEGF11, RP11-536O18.2, F2RL3, AKR1E2, ME3, FABP5, AK7, CD36, RP11-540B6.6, RIN1, PCDH12, RGCC, SDPR, CTD-2319112.4, PRX, RAPGEF4, PRSS23, BAALC, WWTR1, TSPAN12, CABP1, HLX, VWA1, SEMA3F, C16orf80, ITGA6, MPV17L2, AC116035.1, PLVAP, ANKRD65, SH3BP5, RP11- 509E16.1, PASK, PLIN5, FLT1, KIFC3 F.Myofibroblasts SYT10, SOSTDC1, TRDN, RAB9B, NPNT, HSD17B6, RP11-344E13.3, ACTG2, MYOCD, CTB-47B11.3, AF131217.1, TACR2, CNN1, SPOCD1, HHIP, DES, MYH11, ADAMTS6, KCNMB1, MBNL1-AS1, PDLIM3, MFAP5, LTBP1, FAM150A, MYLK, SLC2A4, LUZP2, FAM74A6, ADCY2, FAM168A, RP11-379B18.5, LPP, TMSB15A, ULK2, SMTN, KANK1, FLNA, TAGLN, LMOD1, ARHGEF25, SLMAP, PDLIM7, CAP2, APCDD1, FHL1, TCEAL1, HFE, HHIP-AS1, TGM2, NDUFA4, GRM7, DPEP2, PLN, NEXN, THSD4, LRRC73, NEO1, CSRP1, RP11-611D20.2, PDIA5, CES1, TGFB1I1, TPM2 F.Pcap_Venules SELE, DARC, GAS1, MADCAM1, CCL14, MMRN1, RP11-355F16.1, PLA1A, SNTG2, SELP, MEOX2, ZNF385D, C2CD4B, DUSP23, CSF3, RAB3C, LINC00312, SNORA40, LINC01013, RP4-607J23.2, TUBB3, RP11-782C8.5, CPXM2, SMAD1, IL33, PRCP, PKD1L1, TLL1, LHX6, RP11-417J8.6, SYT15, TSPAN7, GABRD, CACNG8, MED24, RASSF9, ICAM1, REM2, TPD52L1, MEOX1 F.Pericytes FOXS1, NOTCH3, KCNJ8, COX4I2, RGS5, NDUFA4L2, HIGD1B, STEAP4, HEYL, GJC1, CTD-3247F14.2, HRC, LPL, EFHD1, OLFML2B, C1QTNF1, ITGA7, EDNRA, ARVCF, LDB3, FAM162B, RP11-85A1.3, PDGFRB, ENPEP, NR2F2, CTD-3193K9.4, CENPP, HES4, PGF, SEPT4, BGN, AC022007.5, OLFM2, NRIP2, ADCY3, PTGIR, MAP3K7CL, CSRP2, NR1H4, C2orf40, ANO1, SERPINI1, ANGPT2, PLXDC1, LHFP, CYP4X1, HEY2, MEST, TINAGL1, SNAPC3, ADIRF F.Stromal AC002511.2, AC004538.3, AC092652.1, AC116035.1, AC140912.1, ADAM33, ANGPTL1, AP000525.9, BHLHE22, C1QTNF7, C1QTNF9, C1QTNF9B, C22orf31, CAND2, CCDC178, CCDC8, CDO1, CFHR3, CHRD, CHRDL2, CHRM2, CHST1, CLSTN2, COL6A5, CORO6, CTB-92J24.3, CTD-2135D7.5, CTD-2334D19.1, CTD-2536I1.1, CYP1A1, EDNRA, EGFL6, EXOC3L2, FAM155A, FAM162B, FAM171B, FAM19A1, FAM26E, FAM69B, FBXL7, FGF10, FGF14, FIGN, FLRT2, FMO2, FMO3, FNDC1, FOXL1, FOXS1, GALNT15, GALNT16, GIPC3, GJA4, GJA5, GLI2, GLIS1, GLP2R, GPIHBP1, GREM1, GRIA4, GSG1L, HPSE2, HS3ST3A1, IGDCC4, IGF2, IL17B, ITGB3, KCNJ8, KIAA1755, KIRREL, KRT222, KRTDAP, LAMC3, LBP, LHX6, LIFR-AS1, LOXL4, LPHN3, LRCH2, LRRC15, LRRC3B, LYVE1, MAB21L2, MASP1, MATN3, MEOX2, MMRN1, MUSK, MYOCD, NAALAD2, NKX3-2, NOVA2, NPY, NR2F2-AS1, NUDT11, OGN, OMG, PABPC5, PCDHB4, PCDHB7, PGR, PIEZO2, PKNOX2, PLN, PPAPDC1A, PRRX1, PTGFR, PTH1R, RASSF9, RBMS3-AS3, RGMA, RN7SKP295, RNF112, RP11-129B22.1, RP11-152P17.2, RP11- 264B14.1, RP11-395L14.4, RP11-473L15.2, RP11-514D23.3, RP11-536O18.1, RP11-572C15.6, RP11-676J12.6, RP11-710C12.1, RP11-7O14.1, RP11-800A3.7, RP11-804A23.4, RP11-92C4.6, RP3-323P13.2, RSPO2, SALL1, SLC27A6, SLC45A1, SPOCD1, STC2, STRA6, TCEAL5, TEK, TEKT3, TWIST2, VAT1L, VEGFC, WBSCR17, WNT2, ZNF541, ZNF833P, NOTCH3, VSTM2A, CCL21, ASPN, COX4I2, ZNF385D, CTC-276P9.1, CLEC3B, TBX2, DHRS7C, LCN6, KDR, MPDZ, HSPA12B, SFTA1P, MGP, APLNR, PDE1A, SYNDIG1, LMOD1, RAMP3, PAMR1, TNXB, TCF21, FCN3, SRRM3, ZP1, CLDN5, FAM107A, PODN, NTF3, PGM5, RP11- 332H18.4, NR2F1, IL13RA2, DCN, RBPMS2, EMCN, H19, HIGD1B, NKX2-3, AC131025.8, TMEM100, SLIT3, ARHGAP28, DPT, TMTC1, POSTN, OLFML1, PRR16, FENDRR, FOXF2, LINC01082, VWF, FILIP1, PDGFRA, BMP4, AGT, HSPB6, SEMA3E, PCDH19, RP11-449D8.1, CXorf36, PREX2, CXCL14, AC003090.1, COL4A5, CD34, LUM, STMN2, MMRN2, RAET1G, ACSS3, SOSTDC1, AC011526.1, ECSCR, TM4SF18, SVEP1, LIFR, PLVAP, BCL6B, TDO2, NEXN, FAM110D, MFAP5, ELANE, MFAP4, C1QL1, RGS5, SNCG, SNAI2, FAM150B, KIAA1462, DARC, NTN1, GPR63, ACTG2, ACTA2, RBP5, NXN, MADCAM1, PCOLCE, MRVI1, TRIL, TMEM200B, ADORA1, SCARA5, FAM13C, AC124789.1, SEPT4, SULF1, CLEC14A, CDH11, ESAM, PCDH7, CYGB, PCDH18, PLEKHH2, DNM3OS, ADAMTSL3, TMEM119, CCL13, FOXF1, GPR4, CP, FAM167B, ENPP6, GPR116, CCL7, ITGA11, TLL1, EPHA3, COL4A6, ECM2, RAMP2, LPHN2, MIR145, RP11-251M1.1, LOXL1, SGCD, CFH, RP11-736K20.5, FAM19A5, VASN, MMP3, SULT1C4, CAV1, NID1, SELE, SOX17, EFEMP1, IL11, HSD17B6, PDGFRB, PYGO1, HTRA3, CYS1, SHANK3, LRRC17, RASIP1, ADH1B, ADAMDEC1, BICC1, BMP5, CCDC3, RCAN2, TAGLN, NDNF, TAC3, LRRN4CL, SELP, CCDC74B, DIO2, THBS2, GLIS2, C17orf82, FBLN1, HHIP, SEMA3A, MYH11, CAV2, CDH5, COLEC11, CCL11, MMP2, C16orf89, ARHGEF15, RP11-351D16.3, RP11-536O18.2, SGCA, TRAM1L1, DMKN, LTBP2, OSMR, FJX1, COLEC12, GPRC5B, FGF7, ROBO4, AC100830.3, MIR497HG, GLI1, STC1, EDIL3, USHBP1, COL7A1, KCNE4, EGFL7, THSD1, INHBB, CNTN1, COL6A3, HAPLN1, MAPK10, PRICKLE2, PTCH1, PCDHB10, LOX, RP11-157P1.4, MYCT1, MXRA5, EFHD1, TPO, TRPA1, ARHGAP29, TPM2, AHNAK2, BOC, ABLIM3, ADAMTS5, MFAP2, MYOZ3, DCLK1, SOX7, SNCAIP, DCHS1, HMGCLL1, OSR1, AVPR2, AMPH, C14orf37, FLT1, PPAP2B, SYNPO2, SCARF2, SLC9A3R2, PTGDR2, CRISPLD2, SLC16A2, WNT2B, CHODL, LCA5, CNTNAP3B, ADAMTS12, SNED1, RUSC2, PITX1, CFD, CALD1, THY1, CTHRC1, CCL8, TNFRSF10C, RP11-611D20.2, FGF13, HIF3A, FUT1, RP11-23P13.7, WNT5A, FGD5, FAP, MMP11, TRPC6, DACT1, LAMA5, COX7A1, ARHGEF25, JAM2, GGT5, PEAR1, RPS6KA2, LPL, TMEM88, SCUBE1, IGFBP3, CD320, TCF7L1, CACHD1, HOXD3, TFPI, SOX18, MIR143HG, JAG2, TRPC1, TSPAN9, NDUFA4L2, CTD-2314B22.3, HAS1, ARL9, ACKR3, CD248, HOXA11, AASS, CTSK, EVA1A, TNFRSF11B, CTD-2269F5.1, AL590822.1, A2M, NLGN4Y, DES, CCDC80, GRIP2, WNT5B, P4HA3, FBN2, PLAU, EML1, MMP1, FXYD6, MDFI, COL3A1, TM4SF1, RP11-112H10.4, LAMB1, COL9A1, RP11-204M4.2, ADM5, SOD3, CCL14, CLMP, CCL19, NSG1, PPP1R14A, SLC14A1, ROBO1, EMILIN1, RHOJ, MDGA1, C11orf96, ZC3HAV1L, TMEM150C, RP11-486G15.2, F3, CPXM1, RP11-532F6.3, ANGPT1, FGD1, LPAR3, PRKG1, VCAM1, FZD4, SDK1, SCGB1B2P, IGSF9B F.Villus GS1-18A18.1, RP11-804A23.4, REEP2, ENHO, VSTM2A, NPY, PCSK6, FGF9, LPAR3, GSG1L, GLP2R, PTGIS, COL4A5, FAM150B, TTC25, AC002511.2, AC003090.1, CNTFR, AC079779.4, SOX6, BMP5, POSTN, WNT5B, NSG1, PDGFRA, PDGFD, DHRS7C, PTGDR2, RP11-231D20.2, SCUBE1, LANCL2, ZBTB20-AS2, MMP11, DMKN, COL4A6, PTCHD1, EDNRB, C10orf107, RP11-423H2.3, RP4-755D9.1, BMP4, GADD45G, CTC-349C3.1, SEMA3A, KRTDAP, TNFSF15, C1QL1, OBSCN, INSC, F3, APOD F.Villus_1 EFCAB1, TTC25, TSNAXIP1, FAM178B, GDF15 F.Villus_2 RP11-626G11.3, LGALS8-AS1, CTD-2651B20.1, RP11-231D20.2, LPAR3, RP11-834C11.5, AC079779.4, NPY, RP4-794H19.4, ZC3HAV1L, C14orf23, FOLR1

Table 9. All Cell Gene Lists

TABLE 9A Epithelial identE.Absorp- identE.Absorp- identE.Absorp- identE.Absorp- identE.Absorp- tive tive_All tive_TA tive_TA_1 tive_TA_2 identE.Best4_Enterocytes identE.Cycling_TA CA4 C15orf48 C15orf48 LGALS4 COX4I1 BEST4 TUBA1B CEACAM5 C19orf33 LGALS4 C15orf48 LGALS4 CA7 H2AFZ CLDN3 CA2 PHGR1 PIGR C15orf48 SPIB GSTP1 CLDN7 CES2 PIGR KRT8 AGR2 OTOP2 PRDX5 EPCAM CLDN7 TXN MT-ND1 TXN MT1G UBE2C FABP1 EPCAM KRT8 MT-CO3 FABP1 CA4 HMGB2 FTH1 ETHE1 FABP1 EPCAM ATP5G1 MT2A RPS2 FXYD3 FABP1 ATP5G1 MT-CYB MGST1 KRT8 CENPM GUCA2A FXYD3 EPCAM KRT18 ATP5G3 MT1H RPS3 GUCA2B KRT19 AGR2 TXN EPCAM SDCBP2 RPL36A KRT20 KRT8 MT1G MT-ND4 PIGR MT1E RPS5 KRT8 LGALS3 GPX2 MT1G GPX2 KRT19 STMN1 LGALS3 LGALS4 MGST1 MT-CO2 TMSB10 LGALS3 TK1 LYPD8 MT-CO2 MT-ND1 MT-ATP6 COX5B PHGR1 RPLP0 PHGR1 PHGR1 SELENBP1 MT-ND2 PHGR1 KRT20 RPL8 PLAC8 PIGR KRT18 AGR2 CYC1 LYPD8 RPS10 SDCBP2 PRSS3 FXYD3 CLDN7 S100A14 NEURL MIF SRI SDCBP2 MT-CO3 SELENBP1 KRT8 FXYD3 RPL36 TSPAN1 SLC26A2 COX5B GPX2 MT1G LGALS4 PTTG1 CLDN4 SLC26A3 ATP5G3 ATP5G1 URAD FABP1 RPS18 CEACAM1 SRI HMGCS2 PPP1R1B SELENBP1 HES4 RPS9 CEACAM7 TMEM54 CLDN7 PRDX5 COX5A CTSE RPS6 PRSS3 TSPAN1 CHCHD10 COX5B LGALS3 MT1X ATP5G1 AQP8 KRT20 MT-CYB HMGCS2 UGT2B17 EPCAM C17orf76-AS1 C19orf33 MS4A12 CYC1 MT-ND5 CHCHD10 HRCT1 TMSB10 MISP GUCA2A PRDX5 TSPAN8 CA2 S100A10 RPL7A IFI27 SMIM22 MT-ND4 MT-CO1 COX6C CKB RPL35 PRAP1 SELENBP1 PPP1R1B MT1E HMGCS2 ITM2C RPS15 CLCA4 TST MT-CO2 LGALS3 COX6A1 GUCA2A BIRC5 HSD17B2 CHP2 COX5A MGST1 CLDN7 MSLN RPL12 MUC13 KRT18 TSPAN8 CLDN3 TSPO CLDN3 RPS8 LGALS4 CYSTM1 S100A14 CHCHD10 TMEM141 CLDN4 COX4I1 CA2 S100A10 TMSB10 KRTCAP3 TSPAN8 TSPAN1 CENPW CDHR5 CLDN3 COX4I1 ATP5G3 KRT18 SRI HMGB1 S100A10 CA4 TSPO S100A14 FXYD3 KRT18 RANBP1 TMEM54 PKIB LGALS3 KRT19 C10orf99 CLDN7 RPS19 ITM2C C10orf99 CLDN3 ELF3 UQCR10 S100A6 RPL13 CYSTM1 S100A6 KRTCAP3 MT-ND3 C19orf33 DMBT1 HIST1H4C PPDPF TSPAN8 CA2 CA2 SMIM22 MT1M CDKN3 MYO15B CA1 COX6C CYC1 COX6B1 PPDPF RPL10A SMIM22 PLAC8 C10orf99 C10orf99 PPP1R1B C10orf99 AGR2 GPA33 MISP MT1E COX5A UQCRQ TMEM54 CDC20 AOC1 CDHR5 UGT2B17 KLF5 ATP5D CYSTM1 RPL37A S100A6 SLC51B MT-ATP6 COX6C CLDN3 ELF3 IGFBP2 TRIM31 CEACAM7 MT-ND2 MT-RNR1 RPL8 PRSS3 RPSA CDHR2 MT-CO3 TMEM141 ATP5B KRTCAP3 PCSK1N TYMS SPINT2 MT-CO1 ELF3 UGT2B17 KRT19 CEACAM5 AURKB CFDP1 ANPEP KRT19 STARD10 UQCRH C15orf48 RPS21 EMP1 S100A14 ATP5B TSPO ATP5B NOTCH2NL RPS14 MEPIA CKB STARD10 FAM3D AKR1C3 PIGR DTYMK identE.Enterocyte_Immature_1 identE.Enterocyte_Immature_2 identE.Enterocyte_Progenitor ANPEP CA1 CA1 AQP8 CA2 CA2 C19orf33 ETHE1 FABP1 CA4 FABP1 FXYD3 CEACAM5 FXYD3 KRT19 CEACAM7 KRT19 KRT8 CLCA4 KRT20 LGALS4 CTD-2228K2.5 KRT8 PHGR1 FABP1 LGALS3 SELENBP1 FXYD3 MS4A12 C15orf48 GUCA2A PHGR1 CKB GUCA2B SLC26A2 PIGR LYPD8 SLC26A3 LGALS3 MT-CO1 SLC51B SLC26A2 MT-RNR2 TMEM54 CLDN7 PHGR1 SRI KRT18 PLAC8 PLAC8 HSD11B2 PRAP1 MALL CES2 SDCBP2 TSPAN1 ETHE1 SLC26A3 SELENBP1 MT1G TSPAN1 LGALS4 EPCAM CDHR5 CTD-2228K2.5 TSPAN1 CLDN7 C19orf33 C19orf33 MISP PRAP1 UQCRQ MT-RNR1 CEACAM7 TMEM54 MYO15B SDCBP2 S100A14 TRIM31 CKB HMGCS2 IFI27 AKR1B10 MT-CO3 LGALS4 GUCA2A COX5B CEACAM1 TST C10orf99 NEAT1 PKIB MT-CO2 PIGR SLC25A5 CHCHD10 KRT8 GCNT3 ADIRF KRT20 CEACAM1 SMIM22 MT-CO2 MYL6 MT-ND1 CLDN4 CLDN7 CLDN3 SMIM22 CES2 SLC26A3 FTH1 SULT1A2 TST SFN FLNB CHP2 RP11-48O20.4 AQP8 MT-ND4 MS4A12 UQCRQ AMN ELF3 CHP2 ATP5G3 HIST1H1C RP11-48O20.4 MT1E MUC12 ANPEP KRT20 PRSS3 C2orf88 SRI TMEM54 CYSTM1 S100A6 CA2 CDHR5 MT-ND5 SLC51B BSG AKR1C3 AMN IFI27 MT-ATP6 MUC13 COX6A1 MT1M identE.Enterocytes identE.Enteroendocrine identE.Epithelial identE.Goblet identE.Immature_Enterocytes identE.Immature_Goblet ANPEP PCSK1N AGR2 CEACAM5 AQP8 AGR2 APOBEC3B SCGN AMN CLDN4 C15orf48 CLCA1 AQP8 CHGA C10orf99 FAM3D C19orf33 FCGBP C19orf33 CRYBA2 C15orf48 FCGBP CA1 ITLN1 CA4 PYY C19orf33 FXYD3 CA2 KLK1 CEACAM1 FEV CA2 GSN CDHR5 KRT18 CEACAM5 SCG5 CDHR5 IFI27 CEACAM7 LRRC26 CEACAM7 GCG CKB LYPD8 CES2 MUC2 CFDP1 TTR CLDN3 MUC1 CKB REP15 CLCA4 MS4A8 CLDN4 MUC2 CLDN7 RETNLB CLDN23 NEUROD1 CLDN7 TFF1 CTD-2228K2.5 RNASE1 CLDN7 CACNA1A COX5B TFF3 EPCAM SERPINA1 CTD-2228K2.5 STARD10 ELF3 TSPAN1 ETHE1 SPINK1 EMP1 HOXB9 EPCAM ZG16 FABP1 SPINK4 FTH1 MLXIPL FABP1 MUC13 FXYD3 ST6GALNAC1 FXYD3 PRDX5 FAM3D REP15 GUCA2A TFF3 GPRC5A RAB26 FCGBP S100P KRT18 WFDC2 GUCA2A CPE FXYD3 PHGR1 KRT19 ZG16 GUCA2B KIF12 HMGCS2 MT-RNR2 KRT20 LGALS4 HIST1H1C SLC29A4 IFI27 CLDN7 KRT8 TPSG1 HPGD FXYD3 KRT18 ENTPD8 LGALS3 PHGR1 IFI27 CHGB KRT19 ELF3 LGALS4 FXYD3 IL32 SCT KRT20 NEAT1 MALL STARD10 KRT20 VWA5B2 KRT8 KRT18 MISP GMDS LYPD8 MDK LGALS3 MALAT1 MS4A12 KRT8 MISP CES1 LGALS4 SERPINA1 MT-CO2 FAM3D MS4A12 KIAA1324 MT-ATP6 VSIG2 PHGR1 HEPACAM2 MYO15B C15orf48 MT-CO1 PLAC8 PIGR MT-ND1 NLN DDC MT-CO2 LGALS4 PLAC8 RPL36 PKIB HOXB8 MT-CO3 SDCBP2 PRAP1 NPDC1 PLAC8 LGALS4 MT-CYB KLK1 PRSS3 EPCAM PRAP1 ERI3 MT-ND1 TM4SF5 SDCBP2 MB RP11-48020.4 SOX4 MT-ND2 MT-RNR1 SELENBP1 C15orf48 SDCBP2 MARCKSL1 MT-ND4 BCAS1 SLC26A2 SMIM22 SLC26A3 REG4 MT-RNR1 KRT8 SLC26A3 ANG SLC51B TFF3 MT-RNR2 AMN SLC51B ANXA13 SRI KRT8 MT1E CLDN3 SMIM22 MT-CO3 TMEM37 RTN1 MT1G SPATS2L SRI TSPAN13 TRIM31 CXXC4 PHGR1 GUCA2B TMEM54 NANS TSPAN1 TPH1 PIGR SMIM6 TSPAN1 IFI27 TMIGD1 C19orf77 PRSS3 TPSG1 TST CREB3L1 MALL RAMP1 S100A14 CREB3L1 IFI27 COX6C MUC13 SPINK1 S100A6 C19orf33 AMN PRDX5 HSD17B2 ARX SELENBP1 CLTB S100A6 C2orf82 FABP1 DNAJC12 SMIM22 MT-CO1 PKIB RP11-234B24.2 SFN RAB3B SPINT2 MLPH ANPEP SPDEF NEAT1 RP11-279F6.1 TMEM54 SMIM22 CA4 TMEM141 PRSS3 NPDC1 TSPAN1 ZG16B CHP2 TCEA3 MEP1A TMEM141 TSPAN8 CAPN8 MT-CO1 CLDN7 CDA CLDN7 STAP2 EPCAM CYSTM1 URAD identE.Secretory identE.Secretory_AII identE.Secretory_TA identE.Stern identE.Tuft FCGBP CLCA1 TFF3 PRDX5 KRT18 KRT18 FCGBP ITLN1 LEFTY1 AZGP1 MUC2 FXYD3 RPL36 ASCL2 SH2D6 TFF1 ITLN1 KLK1 GPX2 MARCKSL1 TFF3 KLK1 PRDX5 C17orf76-AS1 BIK ZG16 KRT18 SPINK4 RPLP0 LRMP ELF3 KRT8 CLCA1 CDCA7 HCK KRT8 LGALS4 LRRC26 RGMB PTPN18 MT-RNR2 MUC2 MUC2 RPS18 ANXA13 CLDN4 REP15 RETNLB RPL12 KRT8 MUC1 SERPINA1 RPL12 SMOC2 ATP2A3 GSN SPINK1 RPS18 RPS6 AVIL MALAT1 SPINK4 WFDC2 RPS3 IL17RB FXYD3 TFF3 FCGBP PPP1R1B TRPM5 LGALS4 WFDC2 RPL8 GAS5 ALOX5 CEACAM5 ZG16 AGR2 GNB2L1 SH2D7 LYPD8 LRRC26 RPS9 RPS2 BMX MT-CO1 PHGR1 GPX2 MARCKSL1 PTGS1 IFI27 AGR2 RPS2 LGALS4 ELF3 FAM3D TPSG1 RPS3 NUPR1 PPDPF S100P RNASE1 SPINK1 RPS5 EIF1B MT-RNR1 RETNLB RPS15 ETS2 TPM1 TSPAN1 STARD10 ZG16 PIGR GNG13 REP15 MT-ND1 RPS14 RPL29 PSTPIP2 MUC13 FAM3D TMSB10 SLC25A6 MALAT1 S100A6 SMIM22 RPS5 CLDN7 HOTAIRM1 CLDN7 EPCAM PIGR RPL31 SPIB TM4SF5 MT-CO3 C17orf76-AS1 RPS9 TFF3 CLDN3 C15orf48 RPL35 RPL8 CC2D1A PHGR1 MT-ND4 STARD10 EPHB3 HTR3E SERPINA1 ELF3 CLDN7 RPL36A IFT172 SMIM22 CLDN7 RPS8 RPL3 PLCG2 SPATS2L CLDN3 RNASE1 RPL10A DEFB1 ENTPD8 IFI27 LGALS4 RPL5 RASSF6 MT-CO3 NPDC1 RPL18 RPL36 HPGDS MARCKSL1 PIGR RPL37A RPS4X MATK MT-ND4 ST6GALNAC1 RPL13 RPS24 MT-CO3 TPM1 CLDN4 URAD RPL14 MT-CO1 KLK1 MT-CYB MT-ND1 IMPDH2 ANXA4 MT-CO2 MT-ATP6 RPL13A EPCAM PPAP2C BCAS1 MT-ND2 C15orf48 RPL7A AOC1 EPCAM MT-CO1 RPL7A RPL13 OGDHL AZGP1 MT-CO2 REP15 RPS3A ATPIF1 MT-ND5 MARCKSL1 RPS6 RPL13A EPS8L3 PRSS3 MB MT1G ALDH1B1 S100A6 NEAT1 CREB3L1 EPCAM RPS8 FURIN SMIM6 S100A6 RPL32 SLC12A2 H2AFJ ZG16B ANG COX4I1 C15orf48 TMEM63A MT-ND1 MUC1 RPL29 RPS19 IFI6 VSIG2 SPINT2 RPL18A SPINK1 EHF

TABLE 9B Fibroblast identF.Crypt identF.Crypt_RSPO3 identF.Crypt_hiFos identF.Crypt_loFos_1 identF.Crypt_loFos_2 A2M DCN A2M A2M APOE ABCA8 LUM ABCA8 ABCA8 CFD ADAM28 EFEMP1 ADAMDEC1 ADAMDEC1 IGFBP7 ADAMDEC1 FBLN1 APOE APOE IFITM3 ADH1B CFH C1R C1R DCN APOE CFD C1S C1S ADAMDEC1 BMP4 CCDC80 CCL2 CALD1 TMEM176B C1R C1R CCL8 CCL13 FBLN1 C1S C1S CFD CCL2 MFAP4 CALD1 CCL11 COL1A1 CCL8 LUM CCL11 ADH1B COL1A2 CFD SOD3 CCL13 COL1A2 COL3A1 CFH CXCL14 CCL2 CXCL12 COL6A2 CLEC11A A2M CCL8 GSN CTSC COL1A1 C1S CD63 MFAP4 CXCL12 COL1A2 GSN CFD IGFBP7 CXCL14 COL3A1 C1R CFH SOD3 CYGB COL6A2 RARRES2 CLEC11A C7 DCN CTSC LGALS1 COL1A1 SERPINF1 FBLN1 CTSK COL1A2 COL1A2 PLAC9 GPX3 CXCL12 COL3A1 COL3A1 MGP GSN CXCL14 RNA28S5 COL6A1 ADAMDEC1 HAPLN1 CYGB TCF21 COL6A2 SERPING1 IFITM3 DCN CCL13 CTSC TCF21 IGFBP7 DKK3 CTSC CTSK CTSK LUM FBLN1 CCL8 CXCL12 PTGDS MFAP4 GGT5 LTBP4 CXCL14 IFITM3 PPAP2B GPX3 CCL11 CYGB LTBP4 PROCR GSN COL6A2 DCN THY1 RBP1 IFITM3 CD63 DKK3 COL3A1 SERPINF1 IGFBP7 CD81 EFEMP1 RSPO3 SOD3 LGALS1 NGFRAP1 EFEMP2 PMP22 TCF21 LINC01082 RBP1 EMILIN1 VIM TMEM176B LUM TMEM176A FABP4 RARRES2 VIM MFAP4 SELM FBLN1 C3 CALD1 MMP2 PTGDS GGT5 APOE STMN2 PLAC9 CALD1 GNG11 LGALS1 PTN PMP22 COL1A1 GPX3 TMEM176B LINC01082 PPAP2B CCL2 GSN ASPN CTSK PROCR TIMP1 HAAO COL6A2 CCL13 PTN QSOX1 HAPLN1 CALD1 CFH RARRES2 PLAC9 IFITM3 CCL2 PMP22 RBP1 RAB13 IGFBP6 TIMP1 CCL11 SERPINF1 S100A13 IGFBP7 A2M DKK3 SERPING1 CYGB LAPTM4A GPX3 LGALS1 SOD3 GPX3 LGALS1 LAPTM4A SEPP1 SPARC ABCA8 LINC01082 COL14A1 PLAC9 TCF21 PPAP2B LTBP4 PCOLCE GGT5 TIMP1 CST3 LUM DPT RARRES2 TMEM176A CLEC11A MATN2 CD63 SERPING1 TMEM176B VKORC1 identF.Endothelial identF.Endothelial_1 identF.Fibroblast identF.Glia BCAM CD320 A2M ALDH1A1 CAV1 CLDN5 ABCA8 CD9 CCDC85B FABP5 ADAMDEC1 CLU CD320 GNG11 APOE CRYAB CD36 IGFBP4 BMP4 S100B CD59 PLVAP BST2 TUBA1A CLDN5 RAMP2 C1R GPM6B CLEC14A SLC9A3R2 C1S PMP22 CRIP2 CRIP2 CALD1 PLP1 ECSCR SPARCL1 CCL11 SPARC EGFL7 ESAM CCL13 SPP1 ENG EGFL7 CCL2 PRNP ESAM IFITM3 CCL8 SEMA3B FABP5 VAMP5 CD63 JUN FKBP1A GSN CFD MATN2 GIMAP7 TMEM88 CFH FOS GNG11 CD36 CLEC11A CYR61 HLA-C CLEC14A COL1A1 CD59 HLA-E CAV1 COL1A2 COMT IFITM3 RAMP3 COL3A1 IGFBP7 IGFBP4 HLA-E COL6A1 CALM2 IGFBP7 ENPP2 COL6A2 HES1 ITM2B TXNIP CTSC MPZ JAM2 JAM2 CTSK LGALS1 MGP ECSCR CXCL12 ANXA2 NPDC1 SEPW1 CXCL14 LGI4 PLVAP IGFBP7 CYGB GFRA3 RAMP2 CD59 DCN TUBB2B RAMP3 MGP DKK3 CNN3 RBP5 TM4SF1 DMKN C8orf4 SEPW1 BCAM ECM1 PEBP1 SLC9A3R2 NPDC1 EFEMP2 TIMP3 SNCG CCDC85B EID1 DKK3 SPARCL1 VWF EMILIN1 NRXN1 TM4SF1 CD74 FBLN1 IFITM3 TMEM88 GIMAP7 GGT5 TMEM176B VWF ICAM2 GPX3 CCL2 FAM167B FKBP1A GSN IER2 AC011526.1 RBP7 HAAO JUNB SDPR IFITM2 HAPLN1 VIM IFITM2 SDPR IFITM3 EGR1 ENPP2 HLA-C IGFBP6 NDRG2 CYYR1 HLA-DRB1 IGFBP7 RGS16 PRSS23 CYYR1 LAMA4 PMEPA1 GSN ENG LAPTM4A SOCS3 HSPB1 ITM2B LGALS1 RHOB CTGF IFI27 LGALS3BP CBR1 SPARC A2M LINC01082 S100A4 CD34 RBP5 LTBP4 SORBS2 TSPAN7 HES1 LUM AP1S2 identF.Inflammatory identF.Microvascular identF.Myofibrobiasts identF.Pcap_Venules identF.Pericytes NNMT CD320 ACTA2 CLDN5 RGS5 LUM FABP5 TAGLN NPC2 MYL9 C1S PLVAP MYL9 DARC TINAGL1 MMP2 GNG11 TPM2 CLU CSRP2 COL3A1 PRSS23 ACTG2 TSPAN7 NDUFA4L2 IFITM3 CD36 PDLIM3 GNG11 IGFBP7 CXCL14 GSN TPM1 VWF HIGD1B C1R SLC9A3R2 MYLK FABP5 BGN DCN RAMP2 SOSTDC1 RAMP3 COX4I2 IGFBP7 CRIP2 DSTN CPE ADIRF RARRES2 RAMP3 NDUFA4 IGFBP4 FRZB COL1A2 ESAM MYH11 PLVAP TSC22D1 LGALS1 SPARCL1 MYL6 RAMP2 CD36 SPARC VWF FHL1 LY6E SOD3 PLAT VWA1 HHIP ECSCR PDGFRB FBLN1 RGCC PRKCDBP JAM2 TPPP3 TIMP1 ECSCR SELM ITM2B MGP COL1A1 ITM2B LGALS1 EGFL7 NOTCH3 MFGE8 EGFL7 TGFB1I1 SPARCL1 MFGE8 TSPAN4 ENG IGFBP7 CD320 HSPB1 COL6A2 RBP5 CXCL14 MADCAM1 ACTA2 MFAP4 SDPR HSPB1 IGFBP7 IFITM3 COL6A1 VAMP5 TM4SF1 HLA-E EGR1 SERPING1 TMEM88 HSD17B6 APLNR BCAM TMEM176B IGFBP4 DCN CLEC14A GPX3 LY6E FKBP1A FLNA IFITM3 HLA-C PROCR CLEC14A CNN1 DUSP23 CALD1 RBP1 IGFBP7 PPIC HHEX LGALS1 CCL2 CAV1 NPNT CTGF PKIG SOD3 MGP PDLIM7 NNMT HES4 DMKN BCAM COL1A2 NPDC1 CAV1 PLAU SPARC CES1 TM4SF1 PRKCDBP SELM CCDC85B CSRP1 ICAM1 GEM APOE PLAT ILK GIMAP7 ZFP36L1 CALD1 IFITM3 ADAMDEC1 AC011526.1 FAM162B F3 CA4 CAV1 SNCG PGF CTSK TM4SF18 COL3A1 CD74 NR2F2 PKIG TMEM204 LUM CRIP2 TPM2 TPM2 HLA-E PPP1R14A FAM167B MAP1LC3A CTSC HSPG2 SPARC FAM213A EPHX1 A2M EMCN SMTN SDCBP PRSS23 TMEM176A PASK APOE CAV1 CALM2 TCF21 FAM167B C1S TNFSF10 MCAM GPX3 ELTD1 C1R CTNNAL1 STEAP4 PCOLCE SLC14A1 NBL1 HLA-DRB1 GADD45B MYL9 SNCG TMEM176B FKBP1A STOM CYGB PODXL WFDC1 HLA-DRA LHFP WARS FLT1 NEXN GIMAP4 NDUFAF4 RNA28S5 CAV2 SPARCL1 BCAM COL18A1 STMN2 CLDN5 LINC01082 CD34 EPAS1 identF.Stromal identF.Villus identF.Villus_1 identF.Villus_2 A2M AGT CXCL14 BMP4 ADAMDEC1 BMP4 FRZB COL6A2 APOE C1S PLAT CXCL14 BMP4 CALD1 POSTN DMKN BST2 CAV1 DMKN F3 C1R COL1A2 NSG1 FRZB C1S COL3A1 NBL1 MMP2 CALD1 COL6A1 MMP2 NSG1 CCL2 COL6A2 COL6A1 PLAT CCL8 CXCL14 FOS RARRES2 CD63 CYGB CAV1 LGALS1 CFD DMKN VSTM2A COL6A1 CFH EDNRB COL6A2 TMEM176B CLEC11A ENHO TMEM176B POSTN COL1A1 F3 BMP4 ENHO COL1A2 FRZB IGFBP7 IGFBP3 COL3A1 GPX3 F3 IGFBP7 COL6A1 HSD17B2 ENHO IFITM3 COL6A2 IFITM3 CYGB CALD1 CRIP2 IGFBP3 LGALS1 CAV1 CTSC IGFBP7 SDC2 VSTM2A CTSK LGALS1 EDNRB COL3A1 CXCL12 MFAP4 MFAP4 GPX3 CXCL14 MMP2 CALD1 MFGE8 CYGB NBL1 IGFBP3 TPM2 DCN NSG1 RARRES2 TIMP1 ECM1 PLAT GADD45B SDC2 EFEMP2 POSTN GPX3 CYGB EID1 RARRES2 JUNB SPARC EMILIN1 SDC2 TPM2 COL1A2 FBLN1 SERPINF1 SERPINF1 MFAP4 GNG11 SPARC EGR1 HSD17B2 GPX3 TIMP1 HSD17B2 NBL1 GSN TMEM176B IER2 AGT HSPB1 TPM2 SPARC EDNRB IFITM1 VSTM2A IFITM3 FENDRR IFITM3 FOXF1 COL3A1 S100A13 IGFBP6 FENDRR C1S FOXF1 IGFBP7 COL1A1 COL1A2 COL1A1 LAPTM4A SCPEP1 MYL9 C1S LGALS1 MFGE8 HSPA1A SERPINF1 LINC01082 C1R JUN LGALS3BP LTBP4 PPP1R14A AGT SCPEP1 LUM LAPTM4A PDGFD ECM1 MFAP4 ECM1 FOXF1 APLP2 MFGE8 MYL9 ID1 WFDC1 MMP2 PKIG C11orf96 PPP1R14A MYL9 TMEM176A PKIG PKIG NGFRAP1 TMEM119 LAPTM4A C1R NNMT S100A13 FENDRR LTBP4

TABLE 9C Immune identB.Bcells identB.Cycling identB.FO identB.GC identB.Plasma AC096579.7 IGHA1 CD74 CD79A AC096579.7 AL928768.3 IGJ CD79A CD79B AL928768.3 CCR10 CD79A HLA-DRA AL928768.3 CCR10 CD27 AL928768.3 MS4A1 TCL1A CD27 CD74 MZB1 VPREB3 SMIM14 CD79A CD79A DERL3 HLA-DPB1 MS4A1 CHPF DERL3 EAF2 HLA-DRB1 CD74 CRELD2 DNAJB9 IGKC HLA-DPA1 LIMD2 CYTIP EAF2 IGHA2 HLA-DQA1 C7orf10 DERL3 FAM46C TNFRSF17 HLA-DQB1 MARCKSL1 DNAJB9 FCRL5 HERPUD1 CD79B VPREB3 DPP7 FKBP11 UBE2J1 CD37 FCRLA DUSP5 GNG7 SSR4 HERPUD1 IRF8 EAF2 HERPUD1 SEC11C CXCR4 SERPINA9 EVI2B ICAM2 AC096579.7 RPS27 EAF2 FAM46C IGHA1 IGLC2 LTB CD53 FCRL5 IGHA2 DNAJB9 AL928768.3 RGS13 FGF23 IGJ CD74 BANK1 NCF1 FKBP11 IGKC CD27 CD52 BCAS4 GNG7 IGLC2 CCR10 CD83 CD40 GYPC IGLC3 XBP1 LINC00926 SNX29P2 HERPUD1 IGLL5 SDF2L1 RPS23 PTPRCAP ICAM2 MEI1 POU2AF1 IGKC ISG20 IFNAR2 MZB1 FKBP11 RPS25 RHOH IGHA1 PIM2 IGLC3 IGHM CD37 IGHA2 POU2AF1 CYTIP RPL23A POU2AF1 IGJ PTPRCAP MANF RPLP2 LTB IGKC SEC11C GNG7 RPL21 HTR3A IGLC2 SSR4 SPCS3 RP5-887A10.1 HMCES IGLC3 TNFRSF17 PNOC CD19 AC023590.1 IGLL5 UBE2J1 FAM46C FCRLA GPR18 IGLV3-1 SPAG4 DUSP5 SMIM14 CD72 ISG20 CYTIP SSR3 BTG1 HERPUD1 LMAN1 CD79B ISG20 HLA-DMA LAPTM5 MANF EVI2B RGS2 LY86 UBE2J1 MEI1 GYPC IGLL5 RPS8 HMGN1 MZB1 DUSP5 LSP1 PTPRCAP CD22 NUCB2 IGLC7 TRAM1 HLA-DRB5 CD19 PABPC4 TRAM1 CD79B RPS27A LRMP PDIA4 SPCS3 SPCS2 RPS20 NEIL1 PIM2 LSP1 GYPC RPS5 HLA-DMA PPAPDC1B XBP1 PIM2 RPL18A LY86 PRDX4 TPST2 RGS1 RPL32 TPD52 RGCC TXNDC15 CD38 RPL3 IGKC RGS1 CHPF PDIA4 RPL13A HLA-DQA1 SDF2L1 SLAMF7 IFNAR2 FAU CD27 SEC11C PPAPDC1B TPST2 CYBA P2RX5 SLAMF7 PNOC ARHGDIB SELL HLA-DRA SPAG4 IGLV3-1 TSC22D3 HVCN1 HLA-DOB SPCS3 ISG20 CRELD2 RPS3A BASP1 SSR3 identI.Immune identI.Lymphoid identM.CD69neg_Mast identM.CD69pos_Mast identM.Cycling ARHGDIB ARHGDIB TPSAB1 H3F3B TUBA1B CCL5 CCL5 VWA5A NFKBIA AIF1 CD37 CD2 CAPG PPP1R15A FTL CD3D CD3D LTC4S TPSAB1 GPX1 CD3E CD3E KRT1 VWA5A CST3 CD48 CD52 MAOB ANXA1 CD74 CD52 CD69 HPGDS JUN C1QC CD53 CD7 CTSG CTSG HLA-DRB1 CD69 CORO1A GATA2 GLUL LYZ CD7 CYTIP CLU CAPG HLA-DPA1 CORO1A EVL SAMSN1 DNAJA1 MS4A6A CYBA IL32 RP11-354E11.2 UBB C1QA CYTIP LTB FCER1G LMNA HLA-DPB1 EVL PTPRCAP ALOX5AP NFKBIZ HLA-DRA HCST RAC2 SLC18A2 LTC4S C1QB LAPTM5 TRAC FCER1A FTH1 TYROBP LTB TRBC2 NSMCE1 LAPTM4A PSAP PTPRCAP SRGN ANXA1 C1orf186 DNASE1L3 RAC2 IL2RG ADRB2 FCER1G HLA-DQA1 RGS1 LCK BTK HSP90AB1 HLA-DRB5 SRGN CD27 C1orf186 HPGDS NPC2 TRBC2 CD79A GMPR CLU H2AFZ ALOX5AP NKG7 CPA3 DUSP1 FCER1G TRAC HCST ATP6V1F GATA2 HLA-DMA NCF1 CD37 GLUL DDX5 STMN1 TMSB4X SEPT1 TSC22D1 SERPINB1 LST1 COTL1 HOPX SLC45A3 ASAH1 MS4A7 DUSP2 GZMA HS3ST1 BTG2 IGSF6 LCK CD53 SVOPL HSPA1B HLA-DQB1 IL2RG ACAP1 MITF FCER1A TUBB EVI2B RGS1 TYROBP HSPA8 CTSB CKLF PCED1B-AS1 CD9 RPL36AL IL1B IL32 CD48 ALOX5 DNAJB1 HLA-DMB HCLS1 AL928768.3 SDPR HPGD SPI1 CD2 BTG1 LMO4 IER2 CPVL SAMSN1 RPS19 CD44 HDC FAM26F NKG7 TNFRSF17 NCOA4 MAOB VSIG4 PTPRC CTSW FAM212A KRT1 MS4A4A GPSM3 B2M VIM LMO4 RNASE6 HOPX ICAM3 MLPH HSPA5 SAT1 ARPC1B FKBP11 FXYD5 EIF1 CCL3 ACAP1 TSC22D3 S100A11 JUNB AP2S1 ARPC2 RHOH RGS10 EGR1 RNASET2 PCED1B-AS1 TBC1D10C ARHGDIB SLC45A3 NCF4 RHOH IGHV1OR15-1 QPCT RPL7 FGL2 ITGB7 CXCR4 S100A4 DYNLL1 CYBA LIMD2 RPLP1 CATSPER1 MALAT1 LAPTM5 CD27 STK17A ASAH1 SELK CTSH GZMA RPL10 PKM MIR24-2 HLA-DQB2 LCP1 RPL3 LAPTM4A FOSB COTL1 identM.DCs identM.Macrophages identM.Mast identM.Monocytes identM.Myeloid AIF1 ACP5 CAPG ACP5 AIF1 CD74 AIF1 H3F3B AIF1 C1QA CPVL C1QA NFKBIA AMICA1 C1QB CST3 C1QB PPP1R15A C1QA C1QC HLA-DMA C1QC TPSAB1 C1QB CD74 HLA-DMB CD74 VWA5A C1QC CLEC10A HLA-DPA1 CST3 ANXA1 C1orf162 CPVL HLA-DPB1 CTSB GLUL CD74 CST3 HLA-DQA1 CTSD CTSG CLEC10A CTSB HLA-DQB1 CTSZ JUN COTL1 CYBA HLA-DRA CYBA LTC4S CPVL DNASE1L3 HLA-DRB1 DNASE1L3 DNAJA1 CST3 FAM26F HLA-DRB5 FCER1G UBB CTSB FCER1G LST1 FCGRT LMNA CYBA FGL2 LYZ FTL CLU DNASE1L3 FTH1 SPI1 FUCA1 GATA2 FAM26F FTL CLEC10A GPX1 NFKBIZ FCER1G GLUL HLA-DQB2 HLA-DMA LAPTM4A FGL2 GPX1 LGALS2 HLA-DMB FTH1 FTL HLA-DMA AMICA1 HLA-DPA1 C1orf186 GPX1 HLA-DMB COTL1 HLA-DPB1 HSP90AB1 GRN HLA-DPA1 TYROBP HLA-DQA1 HPGDS HLA-DMA HLA-DPB1 FCER1G HLA-DQB1 FCER1G HLA-DMB HLA-DQA1 FCER1A HLA-DRA KRT1 HLA-DPA1 HLA-DQA2 IL1B HLA-DRB1 MAOB HLA-DPB1 HLA-DQB1 HLA-DQA2 HLA-DRB5 ASAH1 HLA-DQA1 HLA-DQB2 MS4A6A IGSF6 FCER1A HLA-DQA2 HLA-DRA CD83 LGMN SERPINB1 HLA-DQB1 HLA-DRB1 DNASE1L3 LST1 DUSP1 HLA-DQB2 HLA-DRB5 GPX1 LYZ BTG2 HLA-DRA IFI30 FGL2 MS4A4A DDX5 HLA-DRB1 IGSF6 SRGN MS4A6A RP11-354E11.2 HLA-DRB5 IL1B C1orf162 MS4A7 HDC IFI30 LST1 ACTB NPC2 SLC45A3 IGSF6 LYZ ITGB2 PSAP IER2 IL1B MPEG1 FAM26F RNASE1 CPA3 ITGB2 MS4A4A MNDA RNASET2 LMO4 LAPTM5 MS4A6A SGK1 S100A11 HSPA8 LGALS1 MS4A7 CFP SAT1 HSPA1B LST1 NPC2 SAT1 SEPP1 HSPA5 LYZ PSAP PLAUR STAB1 HPGD MPEG1 RNASE6 IFI30 TMSB4X SLC18A2 MS4A4A RNASET2 GPR183 TYROBP RPL7 MS4A6A S100A11 RNASET2 CD14 EGR1 MS4A7 SAT1 MPEG1 SDS DNAJB1 NPC2 SPI1 IGSF6 GRN RPL36AL PLAUR SRGN RGS2 CTSS ATP6V1F PSAP TMSB4X LSP1 APOC1 MALAT1 RGS10 TYROBP LY86 SPI1 MIR24-2 RNASE6 VSIG4 RNASE6 AP2S1 CLIC1 RNASET2 SDS identM.Neutrophils identM.Tissue_DCs identM.Tolerogenic_DCs identT.Activated_CD4_hiFos identT.Activated_CD4_loFos CST3 AIF1 CST3 TRBC2 ANXA1 LYZ CD74 CPVL TRAC TRAC AIF1 CLEC10A IDO1 CD69 CD3D LST1 CST3 CD74 ANXA1 LTB HLA-DRB1 HLA-DMA SNX3 CD3D S100A4 HLA-DRA HLA-DPA1 HLA-DPB1 IL32 TRBC2 FTL HLA-DPB1 CLEC9A S100A4 IL32 HLA-DPB1 HLA-DQA1 HLA-DPA1 CD52 CD52 IL1B HLA-DQB1 DNASE1L3 LTB RPLP1 PLAUR HLA-DRA HLA-DRB1 CD2 EEF1A1 TYROBP HLA-DRB1 LGALS2 TSC22D3 ARHGDIB SOD2 LST1 HLA-DRA DNAJA1 RPL10 CD74 LYZ HLA-DQB1 CD3E RPS27A HLA-DPA1 FCER1A HLA-DQA1 ARHGDIB RPS25 FCER1G TYROBP CTD-2319I12.1 KLF6 RPL21 HLA-DQB1 CPVL LYZ BTG1 CD3E GPX1 HLA-DRB5 HLA-DRB5 EIF1 CXCR4 HLA-DRB5 IL1B Clorf54 RPLP1 RPS19 HLA-DMA HLA-DMB HLA-DQB2 HSPA8 RPL32 G0S2 AMICA1 COTL1 SRGN CD2 HLA-DQA1 FCER1G SPI1 CORO1A RPL3 TYMP MS4A6A LSP1 EEF1A1 RPS3 MS4A6A SPI1 IRF8 CCL5 RPS15A SAT1 HLA-DQB2 HLA-DQA2 DUSP1 RPL13 CLEC10A PLAUR AIF1 B2M BTG1 FCN1 LGALS2 MPEG1 YPEL5 RPLP2 SPI1 HLA-DQA2 HLA-DMA TNFAIP3 RPS12 S100A9 GPX1 ACTB TMEM66 RPL9 LGALS2 IGSF6 BATF3 TMSB4X RPS3A CFP CD83 CD83 CXCR4 TMEM66 COTL1 SRGN HLA-DMB ID2 RPS6 CYBA COTL1 SGK1 RGCC CORO1A HLA-DMB CFP FGL2 RPS27A RPS27 NPC2 IFI30 C1orf162 RPL10 TMSB4X SRGN MNDA LST1 PTPRCAP RPL23A IGSF6 DNASE1L3 RGCC H3F3B TPT1 C1orf162 FGL2 RGS10 RPL21 SRGN FAM26F FAM26F CADM1 RPS19 RPL11 CPVL C1orf162 HLA-DOB MYL12A RPSA STX11 ITGB2 PLEK RPS3 RPL19 C1QA RGS2 PPT1 EVL RPS4X FTH1 CD1C HCK DNAJB1 RPS14 FGL2 SAT1 BASP1 IL7R RPL4 ITGB2 RNASE6 PTPRE ACTB GPR183 CTSS GPR183 ITGB2 ZFP36L2 RPS2 OAZ1 CTSH S100B DDX5 B2M MS4A7 SGK1 CST7 RPS25 RPL30 PSAP ACTB GLIPR1 RPL32 RPL28 S100A11 RNASET2 ASB2 SH3BGRL3 RPL31 IFI30 C1QA LY86 JUNB IL7R identT.CD4 identT.CD8 identT.CD8_IELs identT.CD8_LP identT.CXCRB_Th17 identT.Cycling_T identT.ILCs ARHGDIB ACTB CCL5 CCL5 CD2 CD52 LST1 B2M ARHGDIB CD3D NKG7 CD52 STMN1 LTB BTG1 B2M CD52 IL32 CD3D CCL5 KRT86 CD2 CCL5 CD7 DUSP2 LTB CD3D FXYD5 CD3D CD3D HOPX GZMA TRAC CORO1A NFKBIA CD3E CD3E IL32 CD3D TRBC2 IL32 IL4I1 CD52 CD52 NKG7 CCL4 IL32 CD3E ID2 EEF1A1 CD7 TMSB4X B2M S100A4 ARHGDIB CASP3 IL32 CORO1A PTPRCAP TRBC2 CD3E GZMA DUSP1 LTB CTSW GZMA GZMK ID2 TRBC2 ZFP36L1 RPL10 GZMA TRDC BTG1 ARHGDIB HMGB2 TYROBP RPL21 HCST HCST CD8A CXCR6 TUBB EIF1 RPLP1 HOPX CORO1A TRAC KLRB1 TRAC CD52 RPS19 IL32 CD3E TMSB4X ACTB CD2 H2AFY RPS25 NKG7 ACTB CD52 CORO1A ACTB FOS RPS27 PTPRCAP ARHGDIB CXCR4 TMSB4X TYMS HSPA8 RPS27A TMSB4X TRBC2 ARHGDIB CKLF EVL ZFP36 RPS3 TRAC TRGC2 HCST TNFRSF25 KIAA0101 HNRNPA0 TMEM66 TRBC2 CKLF CD8B B2M HMGN2 SPINK2 TMSB4X EVL EVL ZFP36L2 LCK TMSB4X BTG1 TRAC SH3BGRL3 CD160 CD3E SH3BGRL3 LCK BTG2 TRBC2 GZMB RAC2 CD2 CD69 TUBA1B CXCR4 RPL32 CKLF TRAC CST7 GZMA COTL1 IL2RG CORO1A RAC2 CTSW PTPRCAP AC092580.4 PFN1 OTUD5 RPL3 CST7 TMIGD2 HLA-C PTPRCAP RAC2 DDIT4 RPLP2 CD8A KLRC2 CORO1A ARPCIB NKG7 TNFRSF25 RPS15A ID2 GZMB SH3BGRL3 RPS19 TK1 KRT81 RPL13 MYL12A SH3BGRL3 CD7 OSTF1 PTMA ARL4A S100A4 CD8B LCK CD69 HCST CD69 JUNB PTPRCAP CCL4 ABI3 TMEM66 IL2RG PTPRCAP SRGN RPL28 LCK ID2 YPEL5 MYL12A ARPC2 DNAJA1 EIF1 RPS19 ARPC2 EIF1 BTG1 DUT MAFF RPL23A CD160 TRGC1 CTSW PCBP1 H2AFV MIR24-2 RPL19 TRGC2 XCL1 SRGN CACYBP ASF1B TMIGD2 RPS6 CD2 RARRES3 RGCC SPOCK2 HOPX CD69 RPS3A ARPC2 CD96 ACTB GIMAP7 CD7 ALDOC RPL11 CD69 PRF1 HLA-B RPLP1 SRGN LTA4H RPL3O SRGN RPS19 MYL12A SEPT1 B2M FOSB LCK PFN1 AC092580.4 HOPX ODF2L SH3BGRL3 AMICA1 RPL13A RARRES3 STK17A GZMH PFN1 HCST IL7R CXCR4 XCL1 ALOX5AP ID2 CCL5 ARPC1B H3F3B RPS4X ALOX5AP MYL12A H3F3B SLAMF1 SLBP PRMT10 RPL9 TRDC B2M NR4A2 CCL20 H2AFZ IER2 SRGN BTG1 CD247 ANXA1 AMICA1 CKLF SRSF2 RPL4 ZFP36L2 GNLY GZMB CALM1 SRSF7 NR4A2 ANXA1 PRF1 PFN1 EVL CD6 RGS1 EEF1A1 CD69 HLA-C CST7 IL2RG EVL HSPA8 HMGN3 RPSA RPS27 ACTG1 RPS27 ABRACL RRM2 NCOA7 RPL31 DUSP2 TBC1D10C MCL1 EEF1A1 CLSPN YPEL5 RPS2 IL2RG GIMAP7 LCK ARPC2 CTSW NR4A1 identT.MT identT.Memory_CD4 identT.NK identT.PD1_CD4 identT.Tcells identT.Tregs MALAT1 RPS27 NKG7 TRBC2 ACTB IL32 CCL5 RPL21 FCER1G CD3D ARHGDIB TRBC2 MT-CYB BTG1 TYROBP ARHGDIB B2M TRAC SON RPS3 CCL4 TRAC BTG1 BTG1 MT-ND2 RPS25 XCL1 LTB CCL5 ARHGDIB IL32 RPL32 CTSW ITM2A CD2 CD3D MT-ND4 TMEM66 GNLY RP5-1028K7.2 CD3D LTB SF1 RPS27A GZMA CORO1B CD3E B2M VAMP2 RPS15A CD7 ICA1 CD3G RGS1 ARHGEF1 RPL10 GZMK SRGN CD52 SRGN C1orf63 EEF1A1 IL2RB BTG1 CD7 ARPC1B ZFP36L2 RPL3 XCL2 TIGIT CKLF IL2RG FUS RPL13 CLIC3 PTPN7 CORO1A ACTB MT-ATP6 RPLP2 TRDC RPL21 EVL CORO1A ILF3 RPS4X KLRC1 JUNB GZMA CD2 C9orf142 RPS19 GZMB CD200 HCST PFN1 MYH9 RPL9 SRGN LDHB HOPX PTPRCAP SRSF2 RPL19 HCST RPS15A IL2RG CD52 TRABD TRBC2 CCL5 EEF1D IL32 BATF KLF6 RPS20 IFITM2 CD52 LCK CD27 MT-ND5 ARHGDIB KLRD1 COTL1 LTB CREM TSC22D4 RPL31 APOBEC3G RPS4X MYL12A UBC MT-CO3 RPL30 BTG1 CD2 NKG7 RGCC DDX5 RPL23A PRF1 CD27 PTPRCAP TIGIT SSU72 TRAC CST7 RPS15 RAC2 CORO1B ANKRD12 CD52 EIF3G B2M RPLP1 CARD16 SRSF7 RPS3A CCL3 RPS27 RPS19 CD3E TRAPPC1 RPL11 DUSP2 RPL32 RPS27 LCK RBM39 RPL13A HOPX ARPC1B RPS27A UCP2 PPP2R5C RPS6 H3F3B CD3E SH3BGRL3 EIF1 TMEM66 RPS13 CORO1A PTPRCAP TMEM66 RPS27 MIR24-2 RPS14 NR4A2 GIMAP7 TMSB4X S100A4 FOSB RPS12 STK17A CD37 TRAC TMEM66 BTG1 CD3D ZFP36 C9orf16 TRBC2 SPOCK2 ICAM3 LDHB PFN1 LCK PFN1 HLA-A HNRNPK RPL27A ZFP36L2 H3F3B RPL21 TNFRSF4 MT-CO1 RPL4 DUSP1 RPS25 RPS3 RAP1A SUN2 RPL28 CD160 PDCD1 ARPC2 TMSB4X PNISR ZFP36L2 TMSB4X RPL6 SRGN C9orf16 EIF4G2 LTB MATK RPS13 RPLP2 CD44 ABRACL RPL18A CD69 RPL3 SEPT1 RAC2 MRPL20 RPL35A KLRF1 ACTB CD69 BIRC3 HLA-F RPLP1 CD97 RPS27A CD247 TSC22D3 BUB3 RPL41 ARHGDIB RPS3A EEF1A1 EEF1D PRPF38B RPL14 FGR RPL28 ID2 ARPC2 MT-CO2 IL32 ARPC5L RPL7 RPL13 DUSP4 IDS TMSB4X ID2 IL32 ARPC1B HSPA8 PPP1R2 RPS15 MYL12A TMSB4X GIMAP7 PBXIP1 KMT2E RPS18 B2M FXYD5 RPL10 PCBP1 HLA-E RPL7 FAM46C GPSM3 CST7 CALM3

TABLE 10 GWAS Gene List and Cell Subtype MEI1 identB.Plasma SLC26A3 identE.Absorptive_All ITLN1 identE.Immature_Goblet ITLN1 identE.Secretory_All CCL11 identF.Crypt CCDC85B identF.Endothelial CCL11 identF.Fibroblast PROCR identF.Fibroblast CCL2 identF.Stromal EFEMP2 identF.Stromal PROCR identF.Stromal GPX1 identM.Monocytes MXRA8 identF.Stromal SLC26A3 identE.Epithelial PTPRC identI.Immune SEMA3B identF.Glia NKX2-3 identF.Stromal PKIG identF.Stromal FCGR2A identM.Myeloid PLAU identF.Stromal FCGR2A identM.Monocytes CCL11 identF.Stromal VWA1 identF.Microvascular CTSW identI.Immune SULT1A1 identE.Absorptive_All GPR183 identI.Immune SLAMF8 identM.Myeloid SLAMF8 identM.Monocytes HYAL2 identF.Endothelial TAGAP identI.Immune CXCL1 identF.Fibroblast PDLIM4 identF.Stromal SULT1A2 identE.Epithelial ITLN1 identE.Epithelial C1orf106 identE.Epithelial CTSW identT.NK CD6 identT.Tcells LPXN identI.Immune CCL7 identF.Crypt IL10RA identI.Immune RNF186 identE.Epithelial CD19 identB.Bcells MEI1 identI.Immune CREM identI.Immune CXCL1 identF.Stromal TTYH3 identM.Monocytes FUT2 identE.Epithelial ESRRA identE.Epithelial CHP1 identE.Epithelial LY9 identI.Immune HNF4A identE.Epithelial NEU4 identE.Epithelial GSDMB identE.Epithelial PLCG2 identE.Tuft VDR identE.Epithelial CCL7 identF.Fibroblast NEXN identF.Myofibroblasts NEXN identF.Stromal GPR65 identI.Immune SCNN1A identE.Epithelial TNNI2 identM.Myeloid LAMB2 identF.Stromal OVOL1 identE.Epithelial PTPN22 identI.Immune CXCL6 identF.Fibroblast SP140 identI.Immune RSPO3 identF.Crypt_RSPO3 RAPGEF3 identF.Endothelial IKZF1 identI.Immune ANKRD65 identF.Stromal CCL7 identF.Stromal SLC26A6 identE.Epithelial THEMIS identT.Tcells GRB7 identE.Epithelial NLRP7 identB.Bcells CD6 identI.Lymphoid CD28 identT.Tcells MST1R identE.Epithelial CD19 identI.Lymphoid CD6 identI.Immune FADS3 identF.Glia ANKRD65 identF.Microvascular SLAMF8 identI.Immune TAS1R3 identE.Tuft STAT4 identI.Lymphoid TNNI2 identM.Tolerogenic_DCs CXCL6 identF.Stromal SNX20 identI.Immune IFNG identI.Lymphoid SEMA3F identF.Microvascular CD40 identB.GC CD244 identI.Immune CD244 identI.Lymphoid CD19 identI.Immune IFNG identI.Immune HYAL1 identF.Endothelial STAT4 identI.Immune OSMR identF.Stromal SEMA3F identF.Endothelial IRF4 identI.Immune MMEL1 identE.Best4_Enterocytes CIT identF.Microvascular NLRP7 identI.Lymphoid RSPO3 identF.Stromal ITGAL identI.Immune CCR5 identI.Immune TNNI2 identI.Immune DGKE identF.Endothelial IL23R identT.ILCs THEMIS identI.Lymphoid CSF2 identT.ILCs TAS1R3 identE.Secretory THEMIS identI.Immune FAM212A identM.CD69neg_Mast CD28 identI.Immune CD28 identI.Lymphoid TNFRSF9 identT.Tregs CXCR5 identI.Lymphoid MYRF identE.Epithelial BACH2 identB.GC CCR2 identI.Immune NLRP7 identI.Immune CARD11 identI.Immune IL2RA identI.Immune PRKCB identI.Immune RASGRP1 identI.Lymphoid CD226 identI.Immune KIR3DL2 identI.Lymphoid CXCR5 identI.Immune TNFRSF9 identI.Immune CARD11 identI.Lymphoid KIR3DL2 identI.Immune C0L7A1 identF.Stromal CCRL2 identM.Neutrophils IL10 identI.Immune RASGRP1 identI.Immune IKZF3 identI.Lymphoid ACSL6 identT.Tcells RFTN2 identF.Stromal IL27 identM.Monocytes PF4 identE.Epithelial IKZF3 identI.Immune ZMYND10 identM.Cycling IL27 identM.Neutrophils TNFSF8 identI.Immune IL2 identT.Tcells IL23R identI.Lymphoid IL2 identI.Lymphoid CELSR3 identE.Enteroendocrine

Table 11. Specific Cell Gene Lists

TABLE 11A Epithelial identE.Absorp- identE.Absorp- identE.Absorp- identE.Absorp- identE.Absorp- tive tive_All tive_TA tive_TA_1 tive_TA_2 identE.Best4_Enterocytes identE.Cycling_TA CLDN3 C15orf48 TXN MT-ND3 COX4I1 BEST4 MIF CLDN7 CA2 MGST1 SUCLG2 TXN CA7 HIST1H4C EPCAM CES2 UQCRFS1 LCN2 MGST1 OTOP2 IGFBP2 GUCA2A ETHE1 PLA2G2A NGEF ATP5G3 MT1G TUBB4B GUCA2B FABP1 LCN2 DEFA6 CYC1 MT2A RPSAP58 LYPD8 KRT19 ATP5O AC092620.2 TMEM141 MT1H STRA13 PLAC8 LGALS3 SUCLG2 #N/A UQCR10 MT1E CTD-2090113.1 SDCBP2 MT-CO2 CTD-2228K2.7 #N/A ATP5D NEURL CCDC34 CEACAM1 PIGR TLN2 #N/A UQCRH CTSE REG1A ITM2C SLC26A2 PITPNM3 #N/A DBI MT1X RP11-519G16.5 CEACAM6 SLC26A3 XXyac-YM21GA2.4 #N/A COX7C HRCT1 SAPCD2 CLDN23 SRI RP1-102H19.8 #N/A ATP5EP2 MSLN GMNN CA7 KRT20 AC013268.5 #N/A UQCRFS1 DMBT1 C18orf56 TMEM171 MS4A12 CTA-363E6.2 #N/A MESP1 MT1M MZT2B BEST4 GUCA2A AL133245.2 #N/A ATP5O NOTCH2NL NUDT8 NLN SELENBP1 RN7SL485P #N/A BOLA3 MT1F GGCT PRR15L TST RP11-7K24.3 #N/A MRPS33 MYOM1 FOXP1 OTOP2 CHP2 RP11-57H14.4 #N/A CTD-2228K2.7 STAP2 F12 APOBEC3B CYSTM1 CTD-2256P15.4 #N/A GJB1 NBPF10 TOMM40 TMPRSS2 C10orf99 SNORD3B-1 #N/A GOT1 OTOP3 TSFM C12orf36 CA1 FITM1 #N/A MFSD3 GPRC5C CTC-524C5.2 SCIN SLC51B AC007255.8 #N/A APEH CDX1 CDC25C CELA3B CEACAM7 RP11-214N9.1 #N/A LINC00668 SCIN GCAT TDP2 ANPEP RP11-31506.1 #N/A UBAC1 ADCY5 KIF4A CHMP4B S100A14 REG3A #N/A MRPL21 RHOV ATAD3A PTTG1IP CTD-2228K2.5 PLCH1 #N/A SH2D4A TDP2 EMC9 RP11-680F8.1 PRAP1 ATP13A4 #N/A TLN2 CDK18 SNRPF PTPRR PPP1R14D ZSCAN20 #N/A XRCC6BP1 C2orf54 TCOF1 APOBEC1 HMGCS2 CTD-2619J13.14 #N/A C1orf53 CRYL1 NDUFA7 CTSE TMEM45B RP11-192H23.8 #N/A SPRYD4 ALDH2 CECR5 GNG12 SFN #N/A #N/A RP1-102H19.8 CEACAM3 HPDL TRIM15 DHRS11 #N/A #N/A XXyac-YM21GA2.4 NOTCH2 YBX2 MT1H CEACAM1 #N/A #N/A PITPNM3 MEIS1 RCC1 MSLN AKR1B10 #N/A #N/A YY2 CCNYL1 MYO19 TMCC3 AGPAT2 #N/A #N/A ATP13A4 MMEL1 WDR90 B3GNT3 UQCRQ #N/A #N/A RP11-50E11.3 A1CF CTB-175P5.4 CHMP2B SULT1A1 #N/A #N/A CTA-363E6.2 SMPDL3B HMBS HSD17B11 SULT1A2 #N/A #N/A LL22NC03-86G7.1 SULT1E1 SERPINA6 CELA3A STAP2 #N/A #N/A RP11-52112.3 RP11-44N21.1 PTBP1 CTC-490G23.2 AKR1C3 #N/A #N/A RP11-7K24.3 CPA6 PLEK2 DMBT1 MT1G #N/A #N/A UNC79 NBPF14 ACAD9 PARP4 SLC22A18 #N/A #N/A RP11-73M18.9 HR ICT1 RHPN2 TMEM171 #N/A #N/A SNORD3B-1 REN MCM8 MYOM1 ACAA2 #N/A #N/A RP1-80N2.2 RP11-771K4.1 RP11-304L19.1 MT1G TMIGD1 #N/A #N/A RN7SL485P SAMD13 C12orf54 VDAC2 MPST #N/A #N/A RP5-914P20.5 NPY1R RAC3 CEBPA LINC00483 #N/A #N/A HTR4 TNFRSF11A NMRAL1 IL10RB GNA11 #N/A #N/A PLCH1 AGXT TONSL GPRC5C MT1E #N/A #N/A CTD-2256P15.4 TLDC2 C9orf24 C2orf54 SLC22A18AS #N/A #N/A RP11-57H14.4 AC069277.2 POLE identE.Enterocyte_Immature_1 identE.Enterocyte_Immature_2 identE.Enterocyte_Progenitor identE.Enterocytes MT-CO1 ETHE1 SELENBP1 ANPEP MT-RNR1 FABP1 AKR7A3 APOBEC3B MT-CO2 KRT19 GOLM1 AQP8 MT-ND2 KRT20 ACADS C19orf33 MT-ATP6 KRT8 CMBL CEACAM1 MT-ND5 LGALS3 SLC39A5 CEACAM5 MT-ND4L PHGR1 CKMT1B CEACAM7 SIRT6 SLC26A2 CKMT1A CFDP1 VPS13A TMEM54 ASL CLCA4 RP11-747D18.1 LGALS4 TRPM4 CLDN23 SIRT7 AKR1B10 HADH CLDN7 PHYKPL TST SDHA CTD-2228K2.5 BAIAP2L2 SLC25A5 LIMA1 EMP1 MT-TL1 CES2 NAPRT1 FTH1 TAC1 FLNB UGDH GPRC5A KRTAP13-2 UQCRQ BCL2L15 GUCA2A HIST1H3F CHP2 ACO2 HIST1H1C MT-TN BSG AIFM3 IFI27 RP11-505E24.2 COX6A1 PKP2 LYPD8 STAB2 S100A14 MOGAT2 MISP RNU1-134P AHCYL2 ETFA MS4A12 #N/A COX5B OPLAH NLN #N/A SULT1A1 CAPN1 PKIB #N/A PLCD3 OSBPL7 PLAC8 #N/A MGST3 TTLL12 PRAP1 #N/A SLC22A18AS LPIN3 RP11-48020.4 #N/A UQCR11 VPS9D1 SDCBP2 #N/A SGK2 SLC23A1 SLC26A3 #N/A TPRN EME2 SLC51B #N/A TP53I3 TRIM66 SRI #N/A ACAA1 GLDN TMEM37 #N/A ATP1A1 AF127936.7 TRIM31 #N/A ETNK1 C21orf88 TSPAN1 #N/A IGSF9 #N/A TMIGD1 #N/A NDUFA1 #N/A MALL #N/A TNNC2 #N/A SFN #N/A CYP4F12 #N/A PRSS3 #N/A ATP5J #N/A MEP1A #N/A TMEM82 #N/A CDA #N/A LDHD #N/A RHOC #N/A SHD #N/A SMIM22 #N/A ZBTB7B #N/A SULT1A2 #N/A PPARG #N/A ASS1 #N/A RAPGEFL1 #N/A C11orf86 #N/A AXDND1 #N/A SLC6A8 #N/A ITPKA #N/A TMEM171 #N/A MPST #N/A SPINT2 #N/A LETM1 #N/A RHOF #N/A CYCS #N/A GCNT3 #N/A GDPD2 #N/A GPA33 identE.Enteroendocrine identE.Epithelial identE.Goblet identE.Immature_Enterocytes identE.Immature_Goblet PCSK1N AGR2 FAM3D CA1 AGR2 SCGN AMN FCGBP CES2 CLCA1 CHGA C10orf99 MUC1 ETHE1 ITLN1 CRYBA2 C15orf48 MUC2 KRT19 KLK1 PYY C19orf33 TFF1 MT-CO2 LRRC26 FEV CA2 ZG16 PIGR RETNLB SCG5 CDHR5 MUC13 SELENBP1 SERPINA1 GCG CLDN3 REP15 SLC26A2 SPINK1 MS4A8 CLDN4 S100P TST SPINK4 NEUROD1 CLDN7 ENTPD8 CHP2 ST6GALNAC1 CACNA1A COX5B MALAT1 HSD11B2 TFF3 HOXB9 ELF3 VSIG2 FLNB WFDC2 MLXIPL EPCAM TM4SF5 AKR1B10 TPSG1 RAB26 FABP1 BCAS1 SULT1A1 GMDS KIF12 FAM3D AMN MVP HEPACAM2 SLC29A4 FCGBP SPATS2L MGAT4B MB CHGB FXYD3 SMIM6 SLC22A18AS ANG VWA5B2 HMGCS2 CREB3L1 MYO1A TSPAN13 KIAA1324 KRT18 ZG16B PLCD3 NANS DDC KRT19 CAPN8 ATP1A1 RP11-234B24.2 HOXB8 KRT20 FFAR4 GPT TCEA3 ERI3 KRT8 GDPD3 ABCC3 URAD CXXC4 LGALS3 SYTL2 PAPSS2 IL1R2 TPH1 LGALS4 PARM1 CMBL CDC42EP5 C19orf77 MT-ATP6 TBX10 PPARG TSTA3 ARX MT-CO1 FOXA3 SHD RAP1GAP RP11-279F6.1 MT-CO2 LGALS9B IGSF9 TMEM61 ABCC8 MT-CO3 PLA2G10 VIL1 HES6 CADPS MT-ND1 SCNN1A TMPRSS4 FABP2 ETV1 MT-ND4 TP53INP2 CYP4F12 CREB3L4 LCN15 MT-RNR1 BEST2 ACADVL EFCAB4A PELI3 MT1E MLLT3 LETM1 AC011523.2 SST MT1G GALE DGAT1 RAB15 NKX2-2 PHGR1 GPR153 LDHD ERGIC1 PEMT PIGR SPDEF SHROOM1 DYRK4 CYP2W1 PRSS3 SCGB2A1 MAP2K2 CTD-2547H18.1 PAX6 S100A14 AC009133.21 MOGAT3 SNHG18 QDPR SELENBP1 NEDD4L RAPGEFL1 LINC00261 C6orf141 SMIM22 VILL LIMA1 KLK15 COL2A1 SPINT2 RAB27A NAPRT1 PYCR1 BRAT1 TMEM54 DNM2 PACSIN2 C9orf152 SYT13 TSPAN1 FAM101A ITPKA ZNF511 SSTR5-AS1 TSPAN8 GPRIN2 VDR ABLIM1 SEZ6L2 STAP2 FUT3 PFKL KLK4 RXFP4 TFF3 MTMR11 ACO2 GNE PSCA SLC44A4 ACSS2 MMP15 HDLBP KIAA1456 GUCA2A KCNK1 ZBTB7A HES2 MNX1 ETHE1 VIPR1 AXDND1 KDELR2 STX1A TST DST ITGA3 FOXA2 INSL5 PRAP1 RASEF SLC27A4 TRPT1 identE.Secretory identE.Secretory_All identE.Secretory_TA identE.Stem identE.Tuft FCGBP CLCA1 RPL36 PRDX5 KRT18 MUC2 FCGBP RPL35 LEFTY1 AZGP1 TFF1 ITLN1 RPL37A ASCL2 SH2D6 ZG16 KLK1 AC112229.7 GPX2 MARCKSL1 ELF3 KRT18 ANKS6 C17orf76-AS1 BIK MUC1 MUC2 KCNJ12 RPLP0 LRMP MALAT1 REP15 ZSCAN22 CDCA7 HCK S100P SPINK1 FAM183A RGMB PTPN18 TM4SF5 SPINK4 TTC4 RPS18 ANXA13 ENTPD8 TFF3 RP4-610C12.3 RPL12 ATP2A3 BCAS1 WFDC2 KRTAP4-1 SMOC2 AVIL AZGP1 ZG16 RGMB-AS1 RPS6 IL17RB SMIM6 LRRC26 RP11-884K10.7 PPP1R1B TRPM5 ZG16B AGR2 RP11-199F11.2 GNB2L1 ALOX5 SH2D6 TPSG1 SLC25A30-AS1 RPS2 SH2D7 FFAR4 RETNLB B4GALT6 RPS5 BMX CAPN8 STARD10 CTA-797E19.1 RPL29 PTGS1 FOXA3 FAM3D CACNA1F SLC25A6 ELF3 ATP2A3 ST6GALNAC1 AP001462.6 EPHB3 EIF1B TBX10 MB RP11-548H3.1 RPS24 GNG13 SYTL2 CREB3L1 KIAA1875 IMPDH2 PSTPIP2 GALE ANG CITF22-1A6.3 RPL7A HOTAIRM1 LGALS9B MUC1 RP4-565E6.1 ALDH1B1 SPIB GPR153 GMDS SLC35G5 OLFM4 CC2D1A HCK BEST2 RNVU1-14 FERMT1 HTR3E ANXA13 ANXA13 CTD-2196E14.4 AP003774.1 IFT172 AVIL SPDEF CTC-360G5.1 KCNN4 PLCG2 H1F0 FOXA3 ZNF334 EPHB2 DEFB1 RASSF7 ZG16B RP11-677M14.2 GPR160 RASSF6 SCNN1A TFF1 RP11-391M1.4 APEX1 MATK IL17RB CDC42EP5 AP001619.2 PTPRO ANXA4 MLLT3 RP11-234B24.2 LINC00959 RNF186 PPAP2C TRPM5 KIAA1324 ANKUB1 CDK6 AOC1 NEDD4L REG4 CTD-2196E14.6 EXOSC5 OGDHL AC009133.21 TMEM61 RP11-188P20.3 ADCK3 ATPIF1 BMX RAP1GAP CTB-75G16.3 ARSE EPS8L3 SH2D7 S100P AC073133.2 REPIN1 FURIN GNG13 BCAS1 FAM221B ZNF814 TMEM63A FAM101A CAPN9 RP11-932O9.9 NOX1 EHF IFT172 SCGB2A1 HP CDHR1 C2orf82 GPRIN2 TM4SF5 RP11-361F15.2 MACROD1 ESPN HOTAIRM1 AZGP1 OTUB2 SH3YL1 POU2F3 CBFA2T2 ERN2 LRRC16B LGR5 SPTLC2 KCNK1 FFAR4 RP11-163N6.2 UGT2A3 CDH17 EHF ERI3 RP11-13K12.1 SLC39A2 NT5C PSTPIP2 AC009133.21 #N/A ACSM3 BLOC1S1 HTR3E ATP2A3 #N/A SFXN4 IL13RA1 SCGN SH2D6 #N/A LRIG1 CENPV DDR1 TSTA3 #N/A TSPAN6 ASMTL SYT7 ANO7 #N/A CRLS1 FYB

TABLE 11B Fibroblast identF.Crypt identF.Crypt_RSPO3 identF.Crypt_hiFos identF.Crypt_loFos_1 identF.Crypt_loFos_2 A2M DCN ADAMDEC1 APOE IFI27L2 ABCA8 LUM CCL8 SCARA5 PKDCC ADAM28 EFEMP1 HAPLN1 COLEC11 DTX4 ADAMDEC1 FBLN1 STMN2 RP11-54O7.3 ABCA6 APOE CFH CCL7 ANKRD53 C1RL CCL11 CCDC80 IL7 RP11-107N15.1 TEKT3 CCL13 CCL11 EPHA7 LNP1 ROBO1 CCL8 ADH1B PHACTR3 MFI2-AS1 LINC00663 CFD CXCL12 BPI C17orf51 #N/A CFH MFAP4 GALNT9 AC144449.1 #N/A CXCL12 C7 AL117190.3 PNMA2 #N/A DCN SERPINF1 RP11-374M1.5 RN7SKP295 #N/A FABP4 PLAC9 LINC00309 RP11-422P24.11 #N/A FBLN1 SERPING1 LRRC8E L3MBTL1 #N/A HAPLN1 PTGDS ZKSCAN7 FLNC #N/A MFAP4 RSPO3 RP11-556N21.1 ZNF510 #N/A PLTP C3 RP11-88H9.2 LPP-AS2 #N/A PTGDS ASPN RP11-774O3.3 BVES #N/A PTN COL14A1 RP11-353B9.1 DNHD1 #N/A SCARA5 DPT ATP6V0E2-AS1 ZC3H12B #N/A SFTA1P GSTM3 ZNF114 MARK1 #N/A TCF21 GSTM5 MAATS1 RP11-112L6.4 #N/A SNAI2 PRELP C9orf96 RP3-510D11.2 #N/A EDIL3 ANGPTL1 LIN7A SEC24B-AS1 #N/A CXCL1 C16orf89 NBPF15 RP11-267N12.3 #N/A C6orf48 CXCL6 ZNF660 #N/A #N/A TNXB CHODL RP11-326C3.1l #N/A #N/A PROS1 SERPINE2 ANKRD6 #N/A #N/A SERPINE2 OGN CMYA5 #N/A #N/A ABCA6 NFIA PRTG #N/A #N/A IFI27L2 GREM2 RP11-475I24.3 #N/A #N/A CP CCL19 CNTNAP1 #N/A #N/A CCL7 CP WASF1 #N/A #N/A ELANE GPC6 FAM184B #N/A #N/A ANGPTL1 CCL21 DNM3OS #N/A #N/A HOXB-AS3 PAM RP11-173B14.5 #N/A #N/A NR2F1-AS1 RGMA #N/A #N/A #N/A GPC6 APOD #N/A #N/A #N/A CXCL6 RP11-135D11.2 #N/A #N/A #N/A FMOD GPC3 #N/A #N/A #N/A SLIT3 TMEM59 #N/A #N/A #N/A BCL3 PTGER1 #N/A #N/A #N/A CRYBG3 FAIM2 #N/A #N/A #N/A PRCD MAPKAP1 #N/A #N/A #N/A FNDC1 PTGFR #N/A #N/A #N/A EPHA7 SFRP2 #N/A #N/A #N/A CCL19 CAPN6 #N/A #N/A #N/A ADAMTS2 OSR2 #N/A #N/A #N/A RP3-323P13.2 SFRP4 #N/A #N/A #N/A CFHR3 CDO1 #N/A #N/A #N/A identF.Endothelial identF.Endothelial_1 identF.Fibroblast identF.Glia BCAM CD320 ABCA8 ALDH1A1 CCDC85B IGFBP4 ADAMDEC1 CD9 CD320 ENPP2 APOE CLU CD36 TXNIP BMP4 CRYAB CLDN5 ICAM2 C1R S100B CLEC14A RBP7 CIS TUBA1A CRIP2 CYYR1 CCL11 GPM6B ECSCR CD34 CCL13 PMP22 EGFL7 MMRN2 CCL8 PLP1 ENG GPR146 CFD SPARC ESAM IL3RA CFH SPP1 FABP5 SOX17 CLEC11A PRNP FKBP1A SRP14 COL6A1 SEMA3B GIMAP7 FAM107A COL6A2 JUN GNG11 OAZ2 CTSK MATN2 HLA-C C10orf54 CXCL12 FOS HLA-E SYNPO CYGB CYR61 IGFBP4 C10orf10 DCN CD59 ITM2B HEY1 DMKN COMT JAM2 LPAR6 ECM1 CALM2 NPDC1 TIE1 EMILIN1 HES1 PLVAP KLF2 FBLN1 MPZ RAMP2 AIF1L GGT5 ANXA2 RAMP3 ADAM15 HAAO LGI4 RBP5 COL15A1 HAPLN1 GFRA3 SEPW1 NOV LAMA4 TUBB2B SLC9A3R2 PLLP LTBP4 CNN3 SNCG ALPL LUM C8orf4 SPARCL1 SEMA3G MFAP4 PEBP1 TMEM88 BTNL9 MMP2 TIMP3 VWF EFNB2 PCOLCE DKK3 FAM167B MECOM PLAC9 NRXN1 AC011526.1 SHE PROCR CCL2 ENPP2 STC1 PTN IER2 CYYR1 RUNDC3B RARRES2 JUNB PRSS23 C1QTNF9 RBP1 VIM CTGF INHBB SCARA5 EGR1 CD34 FCN3 SERPINF1 NDRG2 TSPAN7 ARL15 SPON2 RGS16 ICAM2 GPIHBP1 STMN2 PMEPA1 PTRF OAZ3 TCF21 SOCS3 VAMP5 RP11-536O18.1 SNAI2 RHOB TGFBR2 SSUH2 ADH1B CBR1 CAV2 PRDM16 PTGDS S100A4 FAM213A FGF12 PLTP SORBS2 EMCN RP11-105C19.1 ADAM28 AP1S2 ELTD1 RP11-1379J22.5 GLT8D2 FXYD1 TM4SF18 SNORA7 TMEM119 ANXA5 HLA-A AC007161.5 VCAM1 S100A1 TXNIP RP4-569M23.2 CTC-276P9.1 PLEKHB1 identF.Inflammatory identF.Microvascular identF.Myofibrobiasts identF.Pcap_Venules identF.Pericytes CHI3L1 FABP5 ACTA2 CLDN5 RGS5 RHBDD3 PLVAP TAGLN NPC2 TINAGL1 RCVRN GNG11 MYL9 DARC CSRP2 MMP3 PRSS23 TPM2 TSPAN7 NDUFA4L2 RP11-676J12.7 CD36 ACTG2 CPE IGFBP7 LRCH2 GSN PDLIM3 LY6E HIGD1B MMP10 RAMP3 TPM1 MADCAM1 BGN AP000688.29 SPARCL1 MYLK APLNR COX4I2 ZC3HAV1L VWF SOSTDC1 DUSP23 ADIRF #N/A VWA1 DSTN HHEX PDGFRB #N/A RGCC NDUFA4 ICAM1 TPPP3 #N/A ITM2B MYH11 TNFSF10 NOTCH3 #N/A ENG MYL6 LINC01013 HES4 #N/A RBP5 FHL1 GPR126 GEM #N/A SDPR HHIP ZNF385D FAM162B #N/A TMEM88 PRKCDBP KCTD12 PGF #N/A FKBP1A TGFB1I1 CCL14 NR2F2 #N/A TM4SF18 HSD17B6 CYP1B1 MCAM #N/A TMEM204 FLNA RPS28 STEAP4 #N/A HSPG2 CNN1 ADM5 STOM #N/A EMCN PPIC PIR LHFP #N/A PASK NPNT LPCAT4 EPS8 #N/A ELTD1 PDLIM7 IL33 SERPINI1 #N/A SLC14A1 CES1 KRT222 REM1 #N/A PODXL CSRP1 SELP ISYNA1 #N/A FLT1 ILK MEOX1 TNS1 #N/A CAV2 SMTN MTUS1 UBA2 #N/A C16orf80 NEXN SEMA6A PLXDC1 #N/A SH3BP5 LINC01082 SMAD1 ADAMTS1 #N/A KDR TCEAL4 GALNT15 ITGA7 #N/A ARHGAP29 HHIP-AS1 VGLL4 NFATC4 #N/A CDC37 C9orf3 ENY2 MEST #N/A APP RBPMS TNFRSF10D EDNRA #N/A RP11-536O18.2 KCNMB1 LEPR NR1H4 #N/A HTRA1 LMOD1 ICAM4 EBF1 #N/A EHD4 CD151 FAM84B OLFM2 #N/A KANK3 PDIA5 RAB3C KCNE4 #N/A CXorf36 UBE2E3 C2CD4B LDB3 #N/A BAALC LPP ZNF521 HEY2 #N/A HLX AOC3 PLA1A HRC #N/A ROBO4 TTLL7 MMP28 RASL12 #N/A NQO1 RCN1 SLC41A3 ARHGEF17 #N/A GAS6 HMG20B FAM155A GJC1 #N/A LXN MIR145 CORT KCNJ8 #N/A SLCO2A1 MFAP5 VEGFC LINC00883 #N/A WWTR1 AC131025.8 CA8 HEYL #N/A GALNT18 PARVA KLK10 C1QTNF1 #N/A MGLL TCEAL1 PRKAR1B FZD7 #N/A PTPRB CALU BCAT1 NTF3 #N/A NRP1 CCDC107 TIAM1 GJA4 identF.Stromal identF.Villus identF.Villus_1 identF.Villus_2 A2M BMP4 POSTN BMP4 ADAMDEC1 COL6A1 NSG1 F3 APOE EDNRB NBL1 IGFBP3 BMP4 ENHO MMP2 APLP2 C1R F3 VSTM2A MMP11 C1S HSD17B2 GADD45B BMP5 CALD1 IGFBP3 PDGFD BAMBI CCL2 MMP2 C11orf96 LANCL2 CCL8 NBL1 LAMA4 TSPAN33 CFD NSG1 PLK2 ITGA8 CFH POSTN CPM NKD2 CLEC11A VSTM2A RBP4 GBGT1 COL1A1 FOXF1 PROM1 BMP7 COL1A2 SCPEP1 SOX6 C22orf31 COL3A1 APLP2 FGF9 RP11-2E17.1 COL6A1 BMP5 TSHZ2 NEFM COL6A2 FAM150B GLP2R LEF1-AS1 CRIP2 PDGFD CRISPLD2 F2RL2 CTSK MMP11 MAFB GRIN2A CXCL12 LAMA4 KLF10 LPAR3 CXCL14 MRPS6 PCSK6 FZD8 CYGB PITX1 FAM92A1 RP11-157P1.4 DCN ISCU SCUBE2 POU6F1 ECM1 C1orf21 NMNAT3 SOX5 EFEMP2 INSC DDHD1 EFHB EMILIN1 RBP4 FRY ARL10 FBLN1 GLP2R RN7SL832P AGAP10 GNG11 GLT8D2 CCDC68 KDM8 GPX3 TSHZ2 FBXO21 RSG1 HSPB1 BAMBI POLA2 RP11-298J20.3 IFITM1 TSLP ADAMTS13 ISPD IFITM3 KREMEN1 AC061992.2 KANSL1L IGFBP6 CRISPLD2 CTD-2035E11.3 #N/A IGFBP7 REEP2 C10orf107 #N/A LINC01082 FGF9 RP11-108M9.6 #N/A LTBP4 TPBG WBSCR17 #N/A LUM LANCL2 HUS1B #N/A MFAP4 PLBD1 EDAR #N/A MFGE8 PCSK6 AP000769.1 #N/A MMP2 SCUBE2 EFCAB1 #N/A MYL9 WNT5B EGOT #N/A NGFRAP1 SEMA4D NOTO #N/A NNMT MFAP2 SRPK3 #N/A PCOLCE LAMA5 RP11-473M20.16 #N/A PLAC9 COL4A6 KCNK17 #N/A PLAT WFS1 ZCCHC18 #N/A PMP22 CCDC68 ZNF410 #N/A PPAP2A SRPX2 BDNF #N/A PPAP2B CNTFR COLGALT2 #N/A PPP1R14A RP11-449D8.1 ZNF594 #N/A

TABLE 11C Immune identB.Bcells identB.Cycling identB.FO identB.GC identB.Plasma identI.Immune identI.Lymphoid AC096579.7 PBK BANK1 CD79A AC096579.7 ARHGDIB CCL5 AL928768.3 SEC23B RP5-887A10.1 CD79B AL928768.3 CCL5 CD2 CCR10 NDC1 SELL TCL1A CCR10 CD37 CD3D CD79A ZBTB8OS ARHGAP24 SMIM14 CHPF CD3D CD3E DERL3 HBD TNFRSF13B MS4A1 CRELD2 CD3E CD52 DNAJB9 ZFAT CCDC50 LIMD2 DERL3 CD48 CD7 EAF2 IGLV3-9 RALGPS2 C7orf10 DNAJB9 CD52 CYTIP FCRL5 KIF14 SIDT1 VPREB3 DUSP5 CD53 EVL GNG7 ZNF264 OSTN-AS1 FCRLA FCRL5 CD69 LTB HERPUD1 ZNF215 FCRL4 SERPINA9 FGF23 CD7 PTPRCAP IGHA1 ZNF66 GYLTL1B EAF2 FKBP11 CORO1A TRAC IGHA2 HIST1H1B CLECL1 CD53 HERPUD1 CYBA TRBC2 IGJ AP000569.9 IGHE NCF1 IFNAR2 CYTIP IL2RG IGKC RP11-166B2.5 DENND5B BCAS4 IGHA1 EVL LCK IGLC2 C4orf21 AP001046.5 CD40 IGHA2 HCST CD27 IGLC3 RP11-382J12.1 BEND4 SNX29P2 IGJ LAPTM5 CD79A IGLL5 HIST1H2AH C2ORF15 ISG20 IGKC LTB NKG7 MEI1 AC090587.5 SMKR1 POU2AF1 IGLC2 PTPRCAP SEPT1 MZB1 CECR7 ZBED2 HTR3A IGLC3 RAC2 HOPX POU2AF1 ACSBG1 KCNIP2 HMCES IGLL5 RGS1 GZMA SEC11C UBE2NL RP11-861A13.4 AC023590.1 IGLV3-1 TRBC2 ACAP1 SSR4 RP4-536B24.3 #N/A CD72 LMAN1 TRAC PCED1B-AS1 TNFRSF17 TTF2 #N/A UBE2J1 MANF NCF1 AL928768.3 UBE2J1 MDH1B #N/A HMGN1 MEI1 COTL1 BTG1 SPAG4 RP11-46H11.12 #N/A NEIL1 MZB1 DUSP2 TNFRSF17 CD79B RP11-266K4.9 #N/A TPD52 PDIA4 LCK CTSW EVI2B DNMT3B #N/A P2RX5 PPAPDC1B IL2RG ICAM3 DUSP5 RP11-347C18.3 #N/A HLA-DOB PRDX4 EVI2B FKBP11 IGLC7 #N/A #N/A BFSP2 SDF2L1 CKLF TSC22D3 SPCS3 #N/A #N/A HVCN1 SEC11C HCLS1 TBC1D10C XBP1 #N/A #N/A GNG7 SPAG4 CD2 IGHV1OR15-1 PPAPDC1B #N/A #N/A EZR SPCS3 SAMSN1 STK17A PNOC #N/A #N/A MTMR14 SSR3 NKG7 POU2AF1 IGLV3-1 #N/A #N/A AICDA SSR4 PTPRC TNFRSF18 FGF23 #N/A #N/A TCEA1 TNFRSF17 GPSM3 FCRL5 CRELD2 #N/A #N/A MBD4 TRAM1 HOPX CD247 TNFRSF13B #N/A #N/A CYB561A3 TXNDC15 ACAP1 MZB1 IGLV6-57 #N/A #N/A RP11-138118.2 WT1-AS ARPC2 DERL3 RP11-290F5.1 #N/A #N/A CD180 XBP1 PCED1B-AS1 CD3G WT1-AS #N/A #N/A CCDC144A IGKV4-1 RHOH CD96 IGHM #N/A #N/A GGA2 IGLV6-57 ITGB7 PIM2 IGKV4-1 #N/A #N/A SEL1L3 IGLC7 LIMD2 GZMB PDIA4 #N/A #N/A BCL7A DNAJB11 CD27 TRDC C16orf74 #N/A #N/A LSM10 SPCS2 GZMA TRGC2 MANF #N/A #N/A TMEM156 ANKRD37 LCP1 TMIGD2 SSR3 #N/A #N/A RP11-164H13.1 ERLEC1 CTSW MEI1 TPD52 #N/A #N/A BACH2 ALG5 TMEM66 TAGAP ANKRD37 #N/A #N/A ZNF581 RP11-290F5.1 FCER1G FAM46C PRDX4 #N/A #N/A CD38 UAP1 CST7 AC092580.4 SPCS2 #N/A #N/A STX7 SPCS1 TBC1D10C GZMM identM.CD69neg_Mast identM.CD69pos_Mast identM.Cycling identM.DCs CAPG H3F3B TUBA1B CD74 LTC4S NFKBIA H2AFZ CPVL KRT1 PPP1R15A STMN1 CST3 MAOB ANXA1 AP2S1 HLA-DPA1 HPGDS GLUL UBE2C HLA-DPB1 SAMSN1 DNAJA1 CENPM HLA-DQA1 ALOX5AP UBB CKS1B HLA-DQB1 SLC18A2 LMNA YWHAH HLA-DRA NSMCE1 NFKBIZ CDK1 HLA-DRB1 ADRB2 C1orf186 ATP6V0B HLA-DRB5 BTK HSP90AB1 KPNA2 CLEC10A GMPR DDX5 NUDT1 HLA-DQB2 SVOPL HDC TOP2A LGALS2 CD44 HSPA5 SNRNP25 AMICA1 NCOA4 FAM46A TROAP FCER1A FAM212A HSP90AA1 EIF4EBP1 HLA-DQA2 CATSPER1 STXBP6 LSM4 SGK1 LYL1 HSPH1 COMMD4 CD1C ARL6IP5 IL1RAPL1 SYCE2 PLD4 HSD17B12 ELF1 GGH CD1E BEX4 UBBP4 NCAPD3 CLEC9A MAML1 AC020571.3 FAM64A PHACTR1 AJ271736.10 DNAJB4 AC009005.2 CD1D NTRK1 RP11-620J15.3 FAM72C IFNGR1 SLC43A3 IL1RL1 ZMYND10 CACNA2D3 PABPC4 EGR3 C20orf201 IDO1 ABCB8 CALB2 SIGLEC15 CTD-2319112.1 IL9R ADCYAP1 GPR42 TNNI2 PSMD1 IL13 RP11-327F22.2 FLT3 CASS4 ARL5B-AS1 INCENP C12orf5 RN7SL243P FER RP11-1100L3.8 SERPINF2 ADAM22 RP11-293M10.2 PIPOX CD207 ASIC4 RP4-794H19.2 RP11-421L21.2 NABP1 RP4-669L17.10 TPSD1 #N/A GHRL RP5-1013A22.5 DKFZP434E1119 #N/A TBC1D9 ACAD11 HIST1H2AG #N/A CLEC4F RP11-336K24.12 #N/A #N/A TATDN3 ST8SIA6 #N/A #N/A DGAT2 ZNF709 #N/A #N/A ELAVL4 #N/A #N/A #N/A XCR1 #N/A #N/A #N/A TOMM34 #N/A #N/A #N/A SLAMF9 #N/A #N/A #N/A UPK3A #N/A #N/A #N/A CD1B #N/A #N/A #N/A SFTPD #N/A #N/A #N/A RFPL4A #N/A #N/A #N/A CEACAM4 #N/A #N/A #N/A AP003774.6 #N/A #N/A #N/A CTD-2514K5.2 #N/A #N/A #N/A CLCN4 identM.Macrophages identM.Mast identM.Monocytes identM.Myeloid identM.Neutrophils identM.Tissue_DCs ACP5 CAPG ACP5 AIF1 IL1B CLEC10A C1QA H3F3B AIF1 C1QA PLAUR FCER1A C1QB NFKBIA C1QA C1QB SOD2 AMICA1 C1QC PPP1R15A C1QB C1QC G0S2 RGS2 CTSB TPSAB1 C1QC CLEC10A TYMP CD1C CTSD VWA5A C1orf162 CPVL FCN1 GPR183 CTSZ ANXA1 CD74 CST3 S100A9 PLD4 FCGRT GLUL CLEC10A CTSB CYBA CD1E FTL CTSG CPVL CYBA STX11 CXCL16 FUCA1 LTC4S CST3 DNASE1L3 OAZ1 CD1D HLA-DMB DNAJA1 CTSB FAM26F C5AR1 PHACTR1 IGSF6 UBB CYBA FTL EREG CACNA2D3 LGMN LMNA DNASE1L3 GLUL CXCL2 LITAF MS4A4A GATA2 FAM26F GPX1 NCF2 P2RY13 MS4A7 NFKBIZ FTL HLA-DPA1 LILRB2 CD207 PSAP C1orf186 GPX1 HLA-DPB1 IL1RN GHRL RNASE1 HSP90AB1 GRN HLA-DQA1 GLRX TBC1D9 RNASET2 HPGDS HLA-DMA HLA-DQA2 CSTA CLEC4F SEPP1 KRT1 HLA-DMB HLA-DQB1 RAB20 ELAVL4 STAB1 MAOB HLA-DPA1 HLA-DQB2 ASGR1 PLB1 TYROBP ASAH1 HLA-DPB1 HLA-DRA S100A8 SLAMF9 CD14 SERPINB1 HLA-DQA1 HLA-DRB1 UBE2D1 CD1B SDS DDX5 HLA-DQA2 HLA-DRB5 ATF5 CEACAM4 GRN RP11-354E11.2 HLA-DQB1 IFI30 JUND RFPL4A APOC1 HDC HLA-DQB2 IGSF6 FCGR1A AP003774.6 SLC40A1 SLC45A3 HLA-DRA IL1B CXCL3 CTD-2514K5.2 GPNMB CPA3 HLA-DRB1 LYZ LILRA2 RP11-667K14.3 PLD3 LMO4 HLA-DRB5 MPEG1 APOBEC3A RASGRF1 FOLR2 HSPA5 IFI30 MS4A4A EMILIN2 TBX19 CD68 HPGD IGSF6 MS4A6A FPR1 RP11-196G11.2 ADORA3 SLC18A2 IL1B MS4A7 SCO2 RUFY4 LIPA RPL36AL LYZ PSAP NLRP3 RP11-13811.2 IGF1 CLIC1 MPEG1 RNASE6 CCRL2 MS4A14 CD163L1 CTNNBL1 MS4A4A RNASET2 ARL8B TMEM170B CSTB DAD1 MS4A6A S100A11 LILRA3 RP11-117D22.2 CREG1 ADRB2 MS4A7 SAT1 RNF19B ZDHHC19 TREM2 ALOX5AP PLAUR SPI1 FCGR1B ANKRD55 MMP12 PLIN2 PSAP TYROBP RP11-701P16.5 RP11-248J18.2 GM2A STX3 RNASE6 VSIG4 IL27 NAMPTL ATOX1 HS3ST1 RNASET2 SDS LILRA5 CTC-428H11.2 CD4 PRKAR1A SAT1 C1orf162 RP11-686D22.8 GRAMD1B ATP6V0D2 HNRNPM SDS ATP6V1F #N/A RP11-147L13.2 CD209 FAM46A SPI1 FCER1A #N/A LEKR1 BRI3 CD44 TYMP TYMP #N/A CTD-2619J13.17 ADAP2 CMA1 TYROBP GRN #N/A LUCAT1 CD163 STXBP6 VSIG4 STAB1 #N/A RP11-73K9.2 DAB2 BTK STAB1 PLAUR #N/A RN7SL605P LILRB5 EIF3D OAZ1 RNF130 #N/A AC144652.1 OTOA SAMSN1 AP2S1 CTSS #N/A RP11-128M1.1 NPL GMPR CTSZ CTSD #N/A #N/A identT.Acti- identT.Acti- identM.Tolerogenic_DCs vated_CD4_hiFos vated_CD4_loFos identT.CD4 identT.CD8 CST3 TSC22D3 RPLP1 RPL10 CCL5 CPVL KLF6 ZDBF2 RPL21 CD8A IDO1 TNFAIP3 AC006369.2 RPLP1 CD8B CD74 CITED2 #N/A RPS25 TRGC2 SNX3 RP11-302B13.5 #N/A RPS27A TRGC1 HLA-DPB1 #N/A #N/A TRAC LYAR CLEC9A #N/A #N/A RPL32 RP11-291B21.2 HLA-DPA1 #N/A #N/A RPS15A NCR2 DNASE1L3 #N/A #N/A RPL19 RP11-713M15.1 LGALS2 #N/A #N/A RPL30 AC131056.3 CTD-2319112.1 #N/A #N/A RPL9 RP11-305L7.3 C1orf54 #N/A #N/A CD40LG SLC25A5-AS1 HLA-DQB2 #N/A #N/A RORA CACNA1C-AS2 COTL1 #N/A #N/A CD5 GSG2 LSP1 #N/A #N/A FLT3LG CCR9 HLA-DQA2 #N/A #N/A CTLA4 #N/A MPEG1 #N/A #N/A PDCD1 #N/A ACTB #N/A #N/A LAIR2 #N/A BATF3 #N/A #N/A RP11-664D1.1 #N/A SGK1 #N/A #N/A SUSD4 #N/A PPT1 #N/A #N/A IL26 #N/A PTPRE #N/A #N/A RP11-265P11.2 #N/A GLIPR1 #N/A #N/A CDKL2 #N/A ASB2 #N/A #N/A HAR1A #N/A KIAA0226L #N/A #N/A AC006369.2 #N/A TMSB4X #N/A #N/A RP4-594110.3 #N/A SERPINF2 #N/A #N/A F5 #N/A TNNI2 #N/A #N/A CCDC157 #N/A SLAMF7 #N/A #N/A LA16c-431H6.6 #N/A FLT3 #N/A #N/A C15orf53 #N/A WDFY4 #N/A #N/A #N/A #N/A SMCO4 #N/A #N/A #N/A #N/A VMO1 #N/A #N/A #N/A #N/A CPNE3 #N/A #N/A #N/A #N/A CKS2 #N/A #N/A #N/A #N/A RAB32 #N/A #N/A #N/A #N/A GSTP1 #N/A #N/A #N/A #N/A FKBP1B #N/A #N/A #N/A #N/A TACSTD2 #N/A #N/A #N/A #N/A CCND1 #N/A #N/A #N/A #N/A C12orf5 #N/A #N/A #N/A #N/A NABP1 #N/A #N/A #N/A #N/A FNIP2 #N/A #N/A #N/A #N/A KIAA1598 #N/A #N/A #N/A #N/A VAC14 #N/A #N/A #N/A #N/A LSM6 #N/A #N/A #N/A #N/A XCR1 #N/A #N/A #N/A #N/A PPM1M #N/A #N/A #N/A #N/A PPM1J #N/A #N/A #N/A #N/A IER5 #N/A #N/A #N/A #N/A identT.CD8_IELs identT.CD8_LP identT.CXCR6_Th17 identT.Cycling_T identT.ILCs identT.MT CCL5 CD8A CD2 TYMS LST1 ACAP1 HOPX CD8B CXCR6 KIAA0101 LTB PAK6 GZMA ZFP36L2 KLRB1 DUT KRT86 CTD-2035E11.5 TRDC GZMH AC092580.4 GINS2 FXYD5 RN7SL55P TRGC2 LYAR SLAMF1 PCNA IL4I1 #N/A KLRC2 IFNG CCL20 DNAJC9 ID2 #N/A ABI3 CRTAM IL12RB1 SMC4 CASP3 #N/A TRGC1 RP11-291B21.2 ZNRD1 MCM3 H2AFY #N/A RARRES3 RP11-305L7.3 ZFYVE28 CENPF HNRNPA0 #N/A CD96 ZNF80 RP11-403A21.1 YEATS4 SPINK2 #N/A CD244 ATP1A3 RP11-85K15.2 NRM OTUD5 #N/A NCR2 #N/A RP11-415F23.2 RAD51 DDIT4 #N/A KIR2DL3 #N/A RP11-401F2.3 CDCA5 ARL4A #N/A RP11-713M15.1 #N/A OVCH1-AS1 TCTEX1D2 ALDOC #N/A DRAXIN #N/A #N/A MTFR2 LTA4H #N/A URB2 #N/A #N/A ACAT2 PRMT10 #N/A RP11-535A5.1 #N/A #N/A VSIG1 SRSF2 #N/A SEC14L6 #N/A #N/A ABCD2 HMGN3 #N/A RP11-104L21.3 #N/A #N/A A1BG MAP3K8 #N/A AL590452.1 #N/A #N/A C5orf17 AREG #N/A ADAMTS17 #N/A #N/A AC027307.3 MPG #N/A SEMA4F #N/A #N/A #N/A IL23R #N/A LRRIQ3 #N/A #N/A #N/A CD164 #N/A KLRC4 #N/A #N/A #N/A CSF2 #N/A ALG11 #N/A #N/A #N/A HINT3 #N/A CCDC7 #N/A #N/A #N/A MED30 #N/A #N/A #N/A #N/A #N/A LINC00299 #N/A #N/A #N/A #N/A #N/A OSTC #N/A #N/A #N/A #N/A #N/A DLL1 #N/A #N/A #N/A #N/A #N/A TNFSF11 #N/A #N/A #N/A #N/A #N/A TCTN3 #N/A #N/A #N/A #N/A #N/A SLC4A10 #N/A #N/A #N/A #N/A #N/A TEX30 #N/A #N/A #N/A #N/A #N/A FXYD7 #N/A #N/A #N/A #N/A #N/A SAMD10 #N/A #N/A #N/A #N/A #N/A PLEKHN1 #N/A #N/A #N/A #N/A #N/A ZNF724P #N/A #N/A #N/A #N/A #N/A ZNF385C #N/A #N/A #N/A #N/A #N/A RP11-403113.5 #N/A #N/A #N/A #N/A #N/A RP11-77P16.4 #N/A #N/A #N/A #N/A #N/A SYDE2 #N/A #N/A #N/A #N/A #N/A RNU2-63P #N/A #N/A #N/A #N/A #N/A RP11-53019.3 #N/A #N/A #N/A #N/A #N/A FAM169A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A #N/A identT.Memory_CD4 identT.NK identT.PD1_CD4 identT .Tcells identT .Tregs RPS27 NKG7 RP5-1028K7.2 CD2 IL32 RPL21 CCL4 CORO1B CD3D TRBC2 RPS25 XCL1 ICA1 CD3E RGS1 RPL32 CTSW PTPN7 CD3G BATF TMEM66 GNLY CD200 LCK CREM RPLP2 IL2RB PDCD1 RPS19 TNFRSF4 RPL9 XCL2 KIF2A TRAC CTLA4 RPL19 CLIC3 RP11-455F5.5 TRBC2 GBP2 RPS20 KLRC1 GNG4 AC092580.4 TNFRSF1B RPL31 GZMB RP11-566E18.3 ACAP1 FOXP3 RPL30 HCST RP11-479G22.8 SIRPG LAIR2 RPL11 KLRD1 RP11-126K1.2 TRGC2 MIR4435-1HG RPL13A APOBEC3G IQSEC3 ICAM3 NINJ2 RPL27A PRF1 NTRK3 RGL4 LINC00649 RPL35A EIF3G #N/A CYTIP TNFRSF9 RPS29 CCL3 #N/A CD8A CUL9 CCR7 STK17A #N/A TIGIT DUSP16 NOSIP CD160 #N/A CXCR6 CDKL2 LEF1 KLRF1 #N/A TRAT1 ANKS1B RP11-664D1.1 FGR #N/A C9orf78 TRAV36DV7 AC013264.2 VPS37B #N/A CD8B RN7SL443P RP11-166B2.3 CMC1 #N/A CD6 C15orf53 #N/A CHST12 #N/A GPR171 TRAV13-2 #N/A LINC00996 #N/A LAG3 TRAV8-2 #N/A SH2D1B #N/A LYAR RP11-53B2.6 #N/A BCO2 #N/A OXNAD1 #N/A #N/A SLC35E1 #N/A DDX24 #N/A #N/A FCRL6 #N/A IGHV1OR15-1 #N/A #N/A RP11-222K16.2 #N/A SSBP4 #N/A #N/A AC017104.6 #N/A RCAN3 #N/A #N/A EOMES #N/A CD40LG #N/A #N/A IL12RB2 #N/A THEMIS #N/A #N/A TRIM54 #N/A RGS14 #N/A #N/A PADI4 #N/A FLT3LG #N/A #N/A RP11-449P15.2 #N/A CD28 #N/A #N/A RP11-24B19.3 #N/A CISH #N/A #N/A KIF21B #N/A CD5 #N/A #N/A #N/A #N/A CA10 #N/A #N/A #N/A #N/A CHRM3-AS2 #N/A #N/A #N/A #N/A BCL11B #N/A #N/A #N/A #N/A UBASH3A #N/A #N/A #N/A #N/A LRRN3 #N/A #N/A #N/A #N/A RP11-291B21.2 #N/A #N/A #N/A #N/A CTLA4 #N/A #N/A #N/A #N/A CCR5 #N/A #N/A #N/A #N/A TNIP3 #N/A #N/A #N/A #N/A MIAT #N/A #N/A #N/A #N/A LINC00649 #N/A #N/A #N/A #N/A AC013264.2 #N/A #N/A #N/A #N/A AC104820.2 #N/A

Tables 12-15 Column Description ident cell subset ID gene gene name contrast DE comparison coefD discrete coefficient of model pvalD discrete p-value coefC continuous coefficient of model pvalC continuous p-value mastfc fold-change of gene estimated by MAST pvalH combined p-value (discrete and continuous) ref name of reference group n number of expressing cells ref_n for reference group alpha fraction of expressing cells ref_alpha for reference group mu mean expression level within expressing cells ref_mu for reference group mean mean expression ref_mean for reference group total fraction of total expression within group ref_total for reference group log2fc log2(fold-change) re1ative to reference group padjD adjusted p-value for discrete term padjC adjusted p-value for continuous term padjH adjusted p-value (combined) contam.res residual from contamination fit contam fraction of total expression within group nsamps number of samples gene is expressed in

TABLE 12 Additional Cell Type Markers ident gene coefD pvalD coefC pvalC mastfc B.Bcells AC096579.7 3.268 0.00E+00 2.04E+00 2.22E−31 2.073248198 B.Bcells AL928768.3 6.364 0.00E+00 9.39E−01 2.47E−04 1.917529901 B.Bcells CD27 3.202 0.00E+00 −5.04E−01  4.30E−13 1.454640372 B.Bcells CD74 4.682 0.00E+00 6.43E−01 1.98E−18 3.951093813 B.Bcells CD79A 7.006 0.00E+00 8.64E−01 3.04E−04 2.727051658 B.Bcells CFL1 −0.738 1.34E−20 −1.64E+00  0.00E+00 −1.184421042 B.Bcells DERL3 4.997 0.00E+00 1.27E+00 1.40E−26 1.221885789 B.Bcells DNAJB9 2.666 0.00E+00 1.02E−01 3.58E−02 1.403867423 B.Bcells FKBP11 2.607 0.00E+00 8.26E−01 1.12E−69 1.333818231 B.Bcells HERPUD1 2.593 0.00E+00 1.74E+00 0.00E+00 2.631118963 B.Bcells IGHA1 2.237  1.67E−211 4.66E+00 0.00E+00 5.929899096 B.Bcells IGHA2 2.087  4.56E−255 4.18E+00 0.00E+00 4.806875561 B.Bcells IGJ 2.338  5.24E−289 4.55E+00 0.00E+00 5.565921598 B.Bcells IGKC 2.917 0.00E+00 4.37E+00  4.37E−196 5.440840209 B.Bcells IGLC2 2.701 0.00E+00 2.24E+00 1.28E−34 2.653469053 B.Bcells IGLC3 2.590 0.00E+00 2.07E+00 3.89E−31 2.686736798 B.Bcells MZB1 4.212 0.00E+00 1.98E+00 3.72E−74 2.231289984 B.Bcells PTPRCAP 2.259  3.03E−294 −9.81E−01  5.62E−61 1.530286416 B.Bcells SEC11C 2.343  8.29E−272 1.01E+00  7.87E−140 1.081174331 B.FO CD74 4.460  2.85E−280 2.49E+00  3.51E−181 5.354121926 B.FO CD79A 3.737 0.00E+00 7.69E−01 1.09E−17 2.695535941 B.FO HLA-DRA 3.473 0.00E+00 1.31E+00 2.57E−31 4.584234603 B.Plasma AC096579.7 4.338 0.00E+00 1.87E+00 1.20E−28 4.119453937 B.Plasma AL928768.3 6.031 0.00E+00 −3.82E−01  4.82E−03 2.80561746 B.Plasma CCR10 5.264 0.00E+00 −3.53E−01  6.29E−03 1.099736317 B.Plasma CD27 4.354 0.00E+00 −6.00E−01  3.05E−17 2.032701947 B.Plasma CD79A 6.105 0.00E+00 −6.42E−01  8.21E−10 2.569609064 B.Plasma CRELD2 3.642 0.00E+00 −7.49E−02  7.62E−02 1.521987695 B.Plasma CYTIP 2.801  8.56E−287 −1.12E+00   4.40E−108 1.172161746 B.Plasma DERL3 7.160 0.00E+00 1.06E+00 1.28E−27 3.432708536 B.Plasma DNAJB9 4.516 0.00E+00 2.31E−01 1.13E−06 2.751694035 B.Plasma DUSP5 3.550 0.00E+00 −5.31E−01  8.87E−15 1.084131907 B.Plasma EAF2 4.763 0.00E+00 −3.45E−01  1.57E−06 1.626266352 B.Plasma EMP3 2.523  1.73E−240 −1.18E+00   4.28E−175 1.039438032 B.Plasma EVI2B 2.894  3.61E−279 −9.89E−01  4.61E−76 1.091108309 B.Plasma FAM46C 3.600 0.00E+00 −6.89E−01  3.30E−41 1.056523747 B.Plasma FGF23 4.651 0.00E+00 −2.47E−01  4.23E−02 1.271037067 B.Plasma FKBP11 5.774 0.00E+00 9.52E−01 3.02E−96 3.37615678 B.Plasma GNG7 4.228 0.00E+00 −5.70E−01  3.94E−21 1.273964782 B.Plasma GYPC 2.905 0.00E+00 −9.97E−01   2.47E−119 1.374166018 B.Plasma HERPUD1 5.656 0.00E+00 1.96E+00 0.00E+00 4.539832048 B.Plasma IGHA1 5.916  8.02E−264 6.74E+00 0.00E+00 8.832840744 B.Plasma IGHA2 5.673 0.00E+00 5.34E+00 0.00E+00 8.005763853 B.Plasma IGJ 6.775 0.00E+00 5.95E+00 0.00E+00 8.446894928 B.Plasma IGKC 4.405 0.00E+00 5.28E+00  2.45E−275 7.801070323 B.Plasma IGLC2 3.773 0.00E+00 2.28E+00 4.98E−32 4.275847217 B.Plasma IGLC3 3.401 0.00E+00 2.02E+00 6.17E−26 3.981855127 B.Plasma IGLL5 4.075 0.00E+00 5.73E−01 6.19E−02 2.106667448 B.Plasma IL2RG 2.386  1.07E−225 −9.48E−01   1.03E−106 1.018567961 B.Plasma ISG20 3.760 0.00E+00 −2.47E−01  5.63E−09 2.1133028 B.Plasma MANF 3.944 0.00E+00 1.73E−01 1.39E−05 2.022112695 B.Plasma MZB1 8.081 0.00E+00 1.70E+00 2.09E−87 4.636645997 B.Plasma NUCB2 2.932  4.18E−299 −4.76E−01  4.17E−31 1.121345488 B.Plasma PDIA4 3.344 0.00E+00 −1.51E−01  2.50E−04 1.089626914 B.Plasma PIM2 3.954 0.00E+00 −6.11E−01  4.80E−16 1.249090523 B.Plasma PPAPDC1B 3.473 0.00E+00 −1.84E−01  9.65E−06 1.180769265 B.Plasma PRDX4 3.794 0.00E+00 2.13E−01 2.49E−08 1.908367774 B.Plasma RGCC 2.955 0.00E+00 −1.39E+00  3.65E−86 1.671612761 B.Plasma RGS1 2.958 0.00E+00 −6.46E−01  3.21E−24 2.027928073 B.Plasma SDF2L1 3.816 0.00E+00 2.29E−01 7.68E−09 2.12000614 B.Plasma SEC11C 5.065 0.00E+00 1.06E+00  1.35E−157 3.257253887 B.Plasma SPCS3 3.550 0.00E+00 −2.48E−01  6.75E−09 1.303454494 B.Plasma SSR3 3.937 0.00E+00 2.78E−01 1.50E−14 1.985908248 B.Plasma SSR4 5.407  2.05E−119 2.36E+00 0.00E+00 4.875540628 B.Plasma TNFRSF17 7.053 0.00E+00 3.55E−01 2.28E−03 2.775933525 B.Plasma TRAM1 3.600 0.00E+00 −3.83E−01  2.34E−25 1.594121993 B.Plasma TXNDC15 3.410 0.00E+00 −3.88E−01  1.71E−18 1.24259521 B.Plasma UBE2J1 4.889 0.00E+00 3.20E−02 5.13E−01 2.040155386 B.Plasma WT1-AS 3.838 0.00E+00 7.54E−01 2.19E−08 1.850996813 B.Plasma XBP1 5.257 0.00E+00 9.96E−01  1.20E−110 3.416010759 E.Absorptive CA4 3.869 0.00E+00 2.23E+00  5.83E−168 4.966152183 E.Absorptive CEACAM5 3.040 0.00E+00 1.32E+00  4.22E−101 2.471517978 E.Absorptive CLDN3 3.520  2.44E−265 7.28E−01 1.38E−70 2.849876849 E.Absorptive CLDN7 3.451  3.17E−254 9.20E−01  2.72E−114 3.239205689 E.Absorptive EPCAM 3.611  8.10E−263 8.16E−01 3.65E−76 3.498387043 E.Absorptive FABP1 4.261  3.07E−269 2.02E+00  1.43E−129 5.705513317 E.Absorptive FTH1 1.212 4.19E−02 2.26E+00 0.00E+00 2.904022981 E.Absorptive FXYD3 4.139  9.84E−269 1.43E+00  1.68E−142 4.637026365 E.Absorptive GUCA2A 3.019 0.00E+00 2.71E+00  2.07E−158 5.019707907 E.Absorptive GUCA2B 2.911 0.00E+00 2.15E+00 2.49E−91 3.832151794 E.Absorptive KRT20 3.141 0.00E+00 9.79E−01 2.09E−53 3.027566969 E.Absorptive KRT8 4.729  1.42E−270 1.04E+00 9.65E−86 4.383298523 E.Absorptive LGALS3 3.504  1.18E−100 1.55E+00  9.06E−244 3.952510867 E.Absorptive LYPD8 3.338 0.00E+00 1.55E+00 2.72E−88 3.510660931 E.Absorptive PHGR1 5.683  1.10E−267 1.69E+00  9.76E−127 5.833162008 E.Absorptive PLAC8 2.520  5.24E−261 1.32E+00 1.29E−80 2.780344753 E.Absorptive SDCBP2 3.592 0.00E+00 1.25E+00  1.13E−118 3.146564742 E.Absorptive SRI 2.653  1.32E−117 1.49E+00  1.05E−263 3.080149952 E.Absorptive TSPAN1 3.255  3.14E−288 1.28E+00  8.98E−120 3.449336247 E.Absorptive_All C15orf48 3.617 0.00E+00 9.36E−01  1.72E−112 3.001269361 E.Absorptive_All C19orf33 2.845 0.00E+00 1.00E+00  5.63E−118 1.314768165 E.Absorptive_All CA2 3.138 0.00E+00 1.71E+00  2.24E−195 2.609090429 E.Absorptive_All CLDN7 3.105 0.00E+00 7.51E−01 4.22E−84 2.010379557 E.Absorptive_All EPCAM 3.213 0.00E+00 4.23E−01 3.37E−23 2.504645735 E.Absorptive_All ETHE1 2.302  2.35E−221 1.03E+00  1.66E−142 1.039913635 E.Absorptive_All FABP1 3.780 0.00E+00 3.21E+00 0.00E+00 5.586554967 E.Absorptive_All FXYD3 3.402 0.00E+00 1.63E+00  9.61E−216 3.576992003 E.Absorptive_All KRT19 2.755 0.00E+00 1.55E+00  8.44E−143 1.818399526 E.Absorptive_All KRT8 3.698 0.00E+00 1.16E+00  6.91E−128 3.836768245 E.Absorptive_All LGALS3 2.848  3.50E−188 1.60E+00 0.00E+00 3.461283056 E.Absorptive_All LGALS4 4.384 0.00E+00 7.03E−01 3.02E−50 4.211537187 E.Absorptive_All PHGR1 5.445 0.00E+00 2.14E+00  9.74E−280 5.851633306 E.Absorptive_All PIGR 3.492 0.00E+00 9.55E−01 5.70E−99 2.40099232 E.Absorptive_All SDCBP2 2.672  5.76E−306 7.80E−01 1.60E−30 1.124968887 E.Absorptive_All SLC26A3 2.567  5.04E−296 1.53E+00 9.49E−54 1.462101925 E.Absorptive_All SRI 2.120  2.05E−168 1.20E+00  2.42E−223 1.743839617 E.Absorptive_All TMEM54 2.793 0.00E+00 9.67E−01  1.34E−104 1.077198575 E.Absorptive_All TSPAN1 2.599  2.92E−308 9.87E−01 1.25E−67 1.638371845 E.Absorptive_TA_1 LGALS4 3.972 0.00E+00 −2.12E−01  4.36E−04 3.560085632 E.Best4_Enterocytes BEST4 5.329 0.00E+00 1.91E+00 8.10E−12 2.425352878 E.Best4_Enterocytes CA7 5.258 0.00E+00 1.69E+00 9.89E−17 2.608165149 E.Best4_Enterocytes SPIB 4.611 0.00E+00 5.00E−01 4.09E−06 1.727259355 E.Enterocyte_Immature_1 ANPEP 3.273 0.00E+00 4.23E−01 3.34E−10 2.255957196 E.Enterocyte_Immature_1 AQP8 5.529 0.00E+00 2.22E+00  6.64E−104 5.678449028 E.Enterocyte_Immature_1 C19orf33 3.309  3.92E−279 7.66E−01 4.51E−54 2.553397084 E.Enterocyte_Immature_1 CA4 4.624 0.00E+00 9.84E−01 2.85E−28 4.39738035 E.Enterocyte_Immature_1 CEACAM5 3.877 0.00E+00 7.92E−01 1.17E−33 2.717411561 E.Enterocyte_Immature_1 CEACAM7 3.601 0.00E+00 2.86E−01 6.89E−05 2.272494617 E.Enterocyte_Immature_1 CLCA4 3.608 0.00E+00 5.71E−01 5.87E−10 1.903154797 E.Enterocyte_Immature_1 CTD-2228K2.5 3.928 0.00E+00 2.35E−01 3.99E−04 2.663088343 E.Enterocyte_Immature_1 FABP1 6.525  1.00E−301 1.58E+00 1.78E−63 5.694861283 E.Enterocyte_Immature_1 FXYD3 5.069 0.00E+00 1.02E+00 1.47E−58 4.485597281 E.Enterocyte_Immature_1 GUCA2A 4.903 0.00E+00 1.94E+00 1.25E−79 5.559428295 E.Enterocyte_Immature_1 GUCA2B 3.889 0.00E+00 8.26E−01 3.33E−16 3.558658878 E.Enterocyte_Immature_1 LYPD8 3.820 0.00E+00 6.53E−01 1.07E−15 3.082198702 E.Enterocyte_Immature_1 MT-RNR2 2.292 2.30E−14 2.71E+00 0.00E+00 4.854022399 E.Enterocyte_Immature_1 PHGR1 5.718  2.20E−275 1.58E+00 1.98E−86 5.828514036 E.Enterocyte_Immature_1 PLAC8 3.821 0.00E+00 9.36E−01 8.51E−43 3.344273115 E.Enterocyte_Immature_1 PRAP1 3.639 0.00E+00 6.96E−01 3.88E−21 2.616769997 E.Enterocyte_Immature_1 SDCBP2 3.416 0.00E+00 5.58E−01 4.57E−22 2.47146566 E.Enterocyte_Immature_1 SLC26A3 3.960 0.00E+00 5.28E−01 9.36E−11 3.105329195 E.Enterocyte_Immature_1 TSPAN1 4.105 0.00E+00 8.49E−01 3.42E−44 3.553346713 E.Enterocyte_Immature_2 CA1 3.617  7.44E−271 1.90E+00 2.14E−95 4.022433153 E.Enterocyte_Immature_2 CA2 6.076  2.56E−210 1.82E+00  5.16E−196 5.018877036 E.Enterocyte_Immature_2 ETHE1 3.172  2.56E−107 1.61E+00  2.65E−288 3.031843788 E.Enterocyte_Immature_2 FABP1 6.700  3.73E−169 3.54E+00 0.00E+00 7.466412634 E.Enterocyte_Immature_2 FXYD3 6.468  3.46E−163 2.11E+00  5.90E−304 5.521904327 E.Enterocyte_Immature_2 KRT19 4.212  5.25E−177 2.29E+00  3.79E−280 4.943887282 E.Enterocyte_Immature_2 KRT20 4.317 0.00E+00 1.31E+00 3.19E−87 3.976800169 E.Enterocyte_Immature_2 KRT8 5.494  7.38E−149 2.01E+00  2.61E−259 5.358446529 E.Enterocyte_Immature_2 LGALS3 3.960 5.85E−49 2.24E+00 0.00E+00 4.773676172 E.Enterocyte_Immature_2 MS4A12 4.243 0.00E+00 1.01E+00 4.80E−42 3.534180442 E.Enterocyte_Immature_2 PHGR1 6.551  1.19E−151 2.63E+00  7.99E−271 6.710120779 E.Enterocyte_Immature_2 SLC26A2 4.441  1.25E−277 1.03E+00 1.22E−65 2.835807204 E.Enterocyte_Immature_2 SLC26A3 4.350 0.00E+00 9.07E−01 2.06E−30 3.660394983 E.Enterocyte_Immature_2 SLC51B 3.934 0.00E+00 4.63E−01 1.35E−17 2.37432504 E.Enterocyte_Immature_2 TMEM54 4.061  8.68E−165 1.39E+00  1.73E−199 3.480691951 E.Enterocyte_Progenitor CA1 3.386 0.00E+00 1.50E+00 8.58E−55 3.281612499 E.Enterocyte_Progenitor CA2 3.952 0.00E+00 8.98E−01 5.54E−42 3.742427108 E.Enterocyte_Progenitor FABP1 6.816 0.00E+00 2.32E+00  2.12E−145 6.384233482 E.Enterocyte_Progenitor FXYD3 4.646 0.00E+00 9.74E−01 2.64E−57 4.403240028 E.Enterocyte_Progenitor KRT19 4.065 0.00E+00 1.24E+00 4.89E−73 3.955605149 E.Enterocyte_Progenitor KRT8 4.971 0.00E+00 1.07E+00 3.04E−69 4.573460965 E.Enterocyte_Progenitor LGALS4 5.934 0.00E+00 1.03E+00 1.02E−70 4.817857244 E.Enterocyte_Progenitor PHGR1 7.475 0.00E+00 1.88E+00  8.07E−133 6.100770415 E.Enterocyte_Progenitor SELENBP1 4.211 0.00E+00 1.33E+00  4.51E−136 3.135115956 E.Enterocytes ANPEP 4.276 0.00E+00 9.70E−01 4.37E−49 3.4334963 E.Enterocytes APOBEC3B 3.764 0.00E+00 6.10E−01 1.70E−21 1.781460279 E.Enterocytes AQP8 7.060 0.00E+00 3.38E+00  2.11E−268 7.177138737 E.Enterocytes C19orf33 5.584  3.11E−198 1.36E+00  2.22E−188 4.137577174 E.Enterocytes CA4 6.565 0.00E+00 2.15E+00  2.95E−149 5.939432428 E.Enterocytes CEACAM1 4.695 0.00E+00 7.73E−01 9.35E−25 3.045247994 E.Enterocytes CEACAM5 6.519 0.00E+00 1.84E+00  4.95E−199 4.700907519 E.Enterocytes CEACAM7 5.715 0.00E+00 9.49E−01 4.29E−43 3.622341305 E.Enterocytes CFDP1 4.497  6.15E−231 1.06E+00  1.38E−132 3.245164922 E.Enterocytes CLCA4 5.018 0.00E+00 1.15E+00 1.95E−32 3.503102339 E.Enterocytes CLDN23 4.089 0.00E+00 5.26E−01 2.60E−16 2.160346928 E.Enterocytes CLDN7 5.365  2.79E−173 1.42E+00  9.21E−207 4.427110007 E.Enterocytes CTD-2228K2.5 5.362 0.00E+00 1.21E+00 9.92E−83 3.877284229 E.Enterocytes EMP1 4.123 0.00E+00 4.12E−01 1.24E−09 2.047517041 E.Enterocytes FTH1 1.916 1.32E−01 3.29E+00 0.00E+00 4.290842634 E.Enterocytes FXYD3 6.057  2.22E−164 1.91E+00  5.88E−195 5.426847174 E.Enterocytes GPRC5A 4.048 0.00E+00 5.24E−01 1.70E−19 1.525511114 E.Enterocytes GUCA2A 6.907 0.00E+00 3.09E+00  6.58E−220 7.354492732 E.Enterocytes GUCA2B 6.330 0.00E+00 1.83E+00 4.32E−82 5.559777218 E.Enterocytes HIST1H1C 4.085 0.00E+00 7.94E−01 2.15E−36 2.894643396 E.Enterocytes HPGD 4.238 0.00E+00 5.12E−01 2.25E−16 2.509509481 E.Enterocytes IFI27 6.392  3.05E−125 2.53E+00 0.00E+00 5.895091164 E.Enterocytes IL32 5.937  3.27E−218 1.59E+00  1.14E−139 4.756889198 E.Enterocytes KRT20 5.007 0.00E+00 8.96E−01 8.40E−40 3.876747723 E.Enterocytes LYPD8 5.363 0.00E+00 1.79E+00  1.38E−122 4.928965265 E.Enterocytes MISP 4.804  3.19E−301 7.87E−01 4.27E−65 2.937076305 E.Enterocytes MS4A12 4.286 0.00E+00 9.91E−01 6.77E−37 3.637728367 E.Enterocytes MY015B 4.284 0.00E+00 3.86E−01 5.87E−14 2.331334816 E.Enterocytes NLN 3.914 0.00E+00 5.51E−01 5.98E−17 1.748615136 E.Enterocytes PKIB 3.969  1.63E−252 1.03E+00 3.43E−94 2.846373547 E.Enterocytes PLAC8 6.696 0.00E+00 2.10E+00  6.90E−230 5.029379735 E.Enterocytes PRAP1 5.954 0.00E+00 1.34E+00 1.28E−81 4.30079732 E.Enterocytes RP11-48020.4 3.959 0.00E+00 5.85E−01 4.40E−29 2.478995999 E.Enterocytes SDCBP2 5.657 0.00E+00 1.52E+00  7.07E−168 4.352042706 E.Enterocytes SLC26A3 5.722 0.00E+00 1.77E+00  1.86E−111 4.84897002 E.Enterocytes SLC51B 3.996 0.00E+00 4.22E−01 1.66E−15 2.404698069 E.Enterocytes SRI 4.171 7.04E−80 1.82E+00  5.05E−295 4.265517134 E.Enterocytes TMEM37 3.713  1.33E−299 6.67E−01 5.75E−41 2.013255733 E.Enterocytes TRIM31 4.538 0.00E+00 4.75E−01 1.39E−11 2.802587786 E.Enterocytes TSPAN1 6.413  1.57E−228 1.94E+00  2.82E−237 5.148729385 E.Epithelial AGR2 3.949 0.00E+00 1.01E+00 8.09E−10 1.253081377 E.Epithelial ANXA1 −4.217 0.00E+00 −1.04E+00  7.40E−07 −1.710241201 E.Epithelial BTG1 −1.582  1.48E−130 −1.36E+00   2.91E−239 −1.367126527 E.Epithelial C15orf48 4.669 0.00E+00 1.59E+00 8.27E−80 2.960253603 E.Epithelial C19orf33 4.647 0.00E+00 9.18E−01 1.35E−10 1.134930377 E.Epithelial CA2 3.288 0.00E+00 1.19E+00 2.03E−32 2.331379028 E.Epithelial CKB 3.289 0.00E+00 8.62E−01 2.47E−12 1.146140076 E.Epithelial CLDN3 4.663 0.00E+00 9.77E−01 1.82E−24 1.215653124 E.Epithelial CLDN4 4.347 0.00E+00 7.77E−01 6.52E−13 1.15526912 E.Epithelial CLDN7 4.624 0.00E+00 1.00E+00 6.15E−31 1.876200849 E.Epithelial COX5B 2.214  5.36E−161 1.11E+00  8.18E−267 1.799641559 E.Epithelial DUSP1 −1.288 2.69E−97 −1.53E+00   2.48E−242 −1.135839708 E.Epithelial EIF1 −1.762 2.34E−66 −1.40E+00  0.00E+00 −2.021194885 E.Epithelial ELF3 4.803 0.00E+00 7.95E−01 2.09E−12 1.239636169 E.Epithelial EPCAM 4.613 0.00E+00 1.62E+00 1.40E−82 2.59722632 E.Epithelial FABP1 3.453 0.00E+00 2.94E+00  3.19E−179 4.955159628 E.Epithelial FCGBP 3.946 0.00E+00 1.37E+00 2.63E−10 1.688693541 E.Epithelial FXYD3 4.263 0.00E+00 2.08E+00  2.40E−125 3.385670825 E.Epithelial H3F3B −1.872 3.49E−99 −1.42E+00  0.00E+00 −1.851301465 E.Epithelial HMGCS2 4.819 0.00E+00 2.68E−01 7.29E−02 1.305286854 E.Epithelial IFI27 2.816 0.00E+00 6.65E−01 1.44E−17 2.137897548 E.Epithelial IFITM2 −2.952 0.00E+00 −1.39E+00  2.78E−77 −1.263956467 E.Epithelial JUNB −1.448 3.67E−98 −1.77E+00  0.00E+00 −1.744661197 E.Epithelial KRT18 4.848 0.00E+00 1.75E+00  9.68E−103 3.014353055 E.Epithelial KRT19 3.783 0.00E+00 1.05E+00 1.11E−15 1.678360125 E.Epithelial KRT20 3.500 0.00E+00 9.49E−01 1.35E−09 1.692310998 E.Epithelial KRT8 4.853 0.00E+00 2.26E+00  2.77E−200 4.101240322 E.Epithelial LGALS1 −3.516 0.00E+00 −1.95E+00  2.98E−52 −1.780792681 E.Epithelial LGALS3 2.748  1.14E−241 1.69E+00  9.68E−287 3.079368421 E.Epithelial LGALS4 5.445 0.00E+00 2.59E+00  5.11E−274 4.781743305 E.Epithelial MT-ATP6 0.934 7.28E−19 2.05E+00 0.00E+00 2.293028029 E.Epithelial MT-ND2 0.492 5.82E−05 1.81E+00 0.00E+00 1.625662978 E.Epithelial MT-RNR1 1.652 3.50E−62 2.20E+00 0.00E+00 3.082297281 E.Epithelial MT1G 3.638 0.00E+00 7.00E−01 7.15E−06 1.243604189 E.Epithelial PIGR 4.870 0.00E+00 1.44E+00 1.80E−40 2.220870574 E.Epithelial RPL21 −2.431 6.34E−73 −1.21E+00   1.28E−260 −3.027643271 E.Epithelial S100A6 2.947  4.26E−150 1.71E+00 0.00E+00 3.608164898 E.Epithelial SMIM22 6.002 0.00E+00 5.78E−01 3.52E−04 1.024792323 E.Epithelial SPINT2 3.019 0.00E+00 7.90E−01 1.76E−51 1.075499988 E.Epithelial TSPAN1 4.132 0.00E+00 1.01E+00 2.20E−11 1.756588332 E.Epithelial ZFP36 −1.608  8.96E−149 −1.59E+00   3.30E−285 −1.438143355 E.Goblet CEACAM5 4.002 0.00E+00 1.03E+00 4.78E−45 2.968738633 E.Goblet CLDN4 3.623  3.64E−260 9.79E−01 4.81E−70 2.991613153 E.Goblet FAM3D 3.571  1.62E−260 8.96E−01 3.82E−68 2.437979965 E.Goblet FCGBP 5.018 0.00E+00 2.85E+00  2.31E−219 5.921268619 E.Goblet FXYD3 4.708  3.13E−259 1.30E+00 6.86E−74 4.686719039 E.Goblet GSN 4.114  1.01E−263 1.45E+00  1.95E−107 4.26091539 E.Goblet IFI27 5.113  2.73E−240 1.79E+00  3.67E−134 5.086890298 E.Goblet LYPD8 4.063 0.00E+00 8.87E−01 2.31E−25 3.43572456 E.Goblet MUC1 3.744  2.28E−303 1.06E+00 8.46E−49 1.779435114 E.Goblet MUC2 6.322 0.00E+00 3.25E+00  1.13E−201 6.142438491 E.Goblet TFF1 5.714 0.00E+00 2.47E+00 3.84E−54 4.455223547 E.Goblet TFF3 5.667 0.00E+00 3.29E+00  5.07E−166 6.864284391 E.Goblet TSPAN1 4.367 0.00E+00 1.20E+00 8.68E−69 4.020758556 E.Goblet ZG16 6.895 0.00E+00 5.45E+00 0.00E+00 9.067037516 E.Immature_Enterocytes AQP8 2.562 0.00E+00 1.17E+00 3.17E−29 2.608741765 E.Immature_Enterocytes C15orf48 3.540 0.00E+00 4.76E−01 3.03E−29 3.057877917 E.Immature_Enterocytes C19orf33 3.153 0.00E+00 7.95E−01 4.84E−85 2.007697328 E.Immature_Enterocytes CA1 2.744 0.00E+00 1.90E+00  4.64E−101 2.192458205 E.Immature_Enterocytes CA2 3.825 0.00E+00 1.35E+00  3.12E−132 3.555364117 E.Immature_Enterocytes CDHR5 2.788 0.00E+00 4.38E−01 4.00E−25 1.143355387 E.Immature_Enterocytes CEACAM7 2.742 0.00E+00 3.30E−01 1.42E−05 1.247437806 E.Immature_Enterocytes CKB 2.424  1.57E−270 1.35E+00  1.05E−108 1.574412494 E.Immature_Enterocytes CLDN7 3.489 0.00E+00 5.32E−01 2.73E−47 2.705758523 E.Immature_Enterocytes CTD-2228K2.5 2.752 0.00E+00 3.71E−01 9.67E−09 1.49783796 E.Immature_Enterocytes EPCAM 2.955 0.00E+00 −1.17E−02  7.87E−01 2.427057509 E.Immature_Enterocytes ETHE1 2.453  4.30E−258 9.99E−01  1.05E−132 1.482997692 E.Immature_Enterocytes FABP1 7.054 0.00E+00 3.05E+00 0.00E+00 6.557149922 E.Immature_Enterocytes FXYD3 4.961 0.00E+00 1.70E+00  1.42E−287 4.711504101 E.Immature_Enterocytes GUCA2A 2.653 0.00E+00 1.35E+00 9.17E−43 2.839818034 E.Immature_Enterocytes KRT18 3.119 0.00E+00 2.67E−01 6.93E−10 2.756402712 E.Immature_Enterocytes KRT19 3.054 0.00E+00 1.74E+00  3.42E−197 2.892412398 E.Immature_Enterocytes KRT20 3.095 0.00E+00 8.75E−01 2.59E−40 2.309331115 E.Immature_Enterocytes KRT8 4.742 0.00E+00 1.46E+00  1.61E−217 4.522895646 E.Immature_Enterocytes LGALS3 3.227  6.30E−211 1.53E+00  3.05E−290 3.780959158 E.Immature_Enterocytes LGALS4 4.998 0.00E+00 6.64E−01 1.01E−44 4.280123818 E.Immature_Enterocytes MS4A12 3.085 0.00E+00 7.42E−01 4.17E−20 1.717936251 E.Immature_Enterocytes PHGR1 6.879 0.00E+00 2.49E+00 0.00E+00 6.287397388 E.Immature_Enterocytes PIGR 3.423 0.00E+00 6.49E−01 5.35E−50 2.774586468 E.Immature_Enterocytes PLAC8 2.738 0.00E+00 5.60E−01 2.45E−18 2.073305121 E.Immature_Enterocytes PRAP1 2.623 0.00E+00 4.30E−01 3.61E−10 1.510711869 E.Immature_Enterocytes SDCBP2 2.707 0.00E+00 3.15E−01 1.19E−09 1.418862701 E.Immature_Enterocytes SELENBP1 2.469  8.53E−272 1.20E+00  7.94E−130 1.298087006 E.Immature_Enterocytes SLC26A2 3.134 0.00E+00 9.92E−01 3.09E−61 1.123729159 E.Immature_Enterocytes SLC26A3 3.427 0.00E+00 8.97E−01 7.27E−31 2.292018359 E.Immature_Enterocytes SLC51B 3.063 0.00E+00 3.81E−01 8.85E−11 1.024945086 E.Immature_Enterocytes SMIM22 2.809 0.00E+00 5.17E−01 4.28E−49 1.685183951 E.Immature_Enterocytes SRI 2.507  5.04E−209 1.08E+00  3.30E−176 2.332610674 E.Immature_Enterocytes TMEM54 2.975 0.00E+00 9.87E−01  2.95E−121 1.645157143 E.Immature_Enterocytes TSPAN1 3.329 0.00E+00 7.60E−01 1.30E−51 2.602637796 E.Immature_Goblet AGR2 3.431  1.31E−304 1.75E+00  4.76E−122 3.413884158 E.Immature_Goblet CLCA1 4.350 0.00E+00 2.34E+00 1.17E−98 3.288406852 E.Immature_Goblet FCGBP 4.495 0.00E+00 2.12E+00  8.68E−176 4.957987636 E.Immature_Goblet ITLN1 5.156 0.00E+00 2.32E+00 3.48E−92 4.367175216 E.Immature_Goblet KLK1 5.385 0.00E+00 1.96E+00  2.94E−163 3.739014763 E.Immature_Goblet KRT18 3.877  1.01E−269 8.78E−01 9.19E−60 3.753416847 E.Immature_Goblet LRRC26 4.285 0.00E+00 8.34E−01 8.76E−29 1.36967859 E.Immature_Goblet MUC2 4.313 0.00E+00 4.61E−01 2.10E−06 3.154373567 E.Immature_Goblet REP15 3.858 0.00E+00 4.12E−01 3.84E−08 1.607019236 E.Immature_Goblet RETNLB 4.214 0.00E+00 1.69E+00 7.13E−42 1.929546104 E.Immature_Goblet RNASE1 4.048 0.00E+00 8.71E−01 3.95E−38 2.827005292 E.Immature_Goblet SERPINA1 3.421 0.00E+00 8.22E−01 3.24E−31 1.633161619 E.Immature_Goblet SPINK1 3.753 0.00E+00 1.08E+00 1.84E−48 1.913114833 E.Immature_Goblet SPINK4 3.885 0.00E+00 1.57E+00 1.52E−19 2.475188133 E.Immature_Goblet TFF3 6.904 0.00E+00 4.93E+00 0.00E+00 8.29841861 E.Immature_Goblet WFDC2 4.563 0.00E+00 1.82E+00 1.43E−85 2.003880612 E.Immature_Goblet ZG16 3.631 0.00E+00 2.46E+00 4.56E−78 5.239192724 E.Secretory FCGBP 2.255  1.76E−180 2.51E+00  2.12E−170 2.685649637 E.Secretory KRT18 3.797 0.00E+00 9.56E−01 2.03E−60 3.870979692 E.Secretory MUC2 3.090  8.90E−300 2.88E+00  1.05E−153 2.97529401 E.Secretory TFF1 3.677 0.00E+00 2.22E+00 2.45E−45 2.433519046 E.Secretory TFF3 3.887 0.00E+00 2.43E+00  7.95E−106 5.096886913 E.Secretory ZG16 2.414  1.69E−209 4.64E+00  6.23E−264 4.51896634 E.Secretory_All CLCA1 3.005 0.00E+00 1.59E+00 1.20E−45 1.398794545 E.Secretory_All FCGBP 3.151 0.00E+00 2.22E+00  4.83E−247 3.402013896 E.Secretory_All FXYD3 2.648  7.25E−302 −6.63E−01  6.00E−37 2.27714686 E.Secretory_All ITLN1 3.479 0.00E+00 1.50E+00 5.99E−33 1.898258706 E.Secretory_All KLK1 4.279 0.00E+00 1.28E+00 5.36E−62 1.43230919 E.Secretory_All KRT18 3.810 0.00E+00 8.00E−01 1.08E−74 3.69599281 E.Secretory_All KRT8 3.729 0.00E+00 −1.29E−01  7.04E−03 3.307698873 E.Secretory_All LGALS4 3.259 0.00E+00 3.38E−02 4.74E−01 3.402953324 E.Secretory_All MUC2 3.811 0.00E+00 1.65E+00 7.54E−54 2.531118742 E.Secretory_All REP15 3.631 0.00E+00 5.12E−01 1.68E−07 1.007908306 E.Secretory_All SPINK4 3.264 0.00E+00 7.97E−01 2.70E−05 1.333729761 E.Secretory_All TFF3 4.523 0.00E+00 4.34E+00 0.00E+00 6.403931399 E.Secretory_All ZG16 2.819 0.00E+00 3.35E+00  1.31E−190 4.477100018 E.Tuft KRT18 5.434  7.28E−158 2.62E+00  1.91E−209 5.752838414 F.Crypt A2M 4.284 0.00E+00 1.17E+00 1.85E−72 3.492074115 F.Crypt ABCA8 5.496 0.00E+00 7.50E−01 5.75E−06 1.688536779 F.Crypt ADAM28 3.648 0.00E+00 7.34E−01 1.73E−17 1.3316427 F.Crypt ADAMDEC1 5.668 0.00E+00 4.47E+00 0.00E+00 5.70918829 F.Crypt ADH1B 3.617 0.00E+00 1.26E+00 1.14E−43 1.243902457 F.Crypt APOE 6.298 0.00E+00 3.31E+00 0.00E+00 6.688838049 F.Crypt BMP4 3.215 0.00E+00 −5.22E−01  6.37E−13 1.570952671 F.Crypt C1R 5.051 0.00E+00 1.27E+00 6.77E−60 3.743899141 F.Crypt C1S 5.165 0.00E+00 1.18E+00 2.98E−50 3.879547488 F.Crypt CALD1 3.961 0.00E+00 1.27E−01 7.55E−02 2.800815759 F.Crypt CCL11 5.288 0.00E+00 2.77E+00 9.04E−12 3.068255858 F.Crypt CCL13 5.690 0.00E+00 3.29E+00 1.88E−14 2.738743783 F.Crypt CCL2 4.486 0.00E+00 1.01E+00 7.78E−15 3.492339648 F.Crypt CCL8 5.709 0.00E+00 2.86E+00 1.14E−33 2.701919577 F.Crypt CD63 2.718  4.96E−122 1.43E+00 0.00E+00 3.486481313 F.Crypt CFD 6.712 0.00E+00 4.21E+00 0.00E+00 6.838074558 F.Crypt CFH 4.252 0.00E+00 6.33E−01 7.26E−09 1.853771933 F.Crypt CLEC11A 3.606 0.00E+00 5.62E−01 1.03E−18 1.895949104 F.Crypt COL1A1 4.065 0.00E+00 1.86E−01 3.22E−02 2.600863122 F.Crypt COL1A2 4.802 0.00E+00 5.71E−01 1.78E−13 3.478176115 F.Crypt COL3A1 4.651 0.00E+00 6.79E−01 1.20E−13 3.464081884 F.Crypt COL6A1 3.150 0.00E+00 −4.52E−01  3.79E−10 1.63183674 F.Crypt COL6A2 4.071 0.00E+00 −1.23E−01  1.12E−01 2.870797734 F.Crypt CTSC 3.442 0.00E+00 2.00E+00 0.00E+00 3.77792912 F.Crypt CTSK 4.270 0.00E+00 6.12E−01 9.43E−11 2.07068938 F.Crypt CXCL12 4.295 0.00E+00 8.91E−01 2.89E−17 2.357940547 F.Crypt CXCL14 3.894 0.00E+00 2.81E+00 0.00E+00 5.192128961 F.Crypt CYGB 4.307 0.00E+00 3.91E−02 6.32E−01 2.398157949 F.Crypt DCN 6.004 0.00E+00 2.79E+00  2.10E−201 4.989098789 F.Crypt DKK3 4.247 0.00E+00 −2.46E−01  1.45E−02 1.25655402 F.Crypt EFEMP1 4.062 0.00E+00 3.40E−01 2.66E−02 1.037851843 F.Crypt EFEMP2 3.540 0.00E+00 −4.70E−02  5.51E−01 1.084607071 F.Crypt EMILIN1 3.650 0.00E+00 6.55E−02 4.18E−01 1.522259058 F.Crypt FABP4 5.111 0.00E+00 2.30E−01 5.01E−01 1.194045652 F.Crypt FBLN1 5.764 0.00E+00 1.54E+00 1.40E−46 3.438001639 F.Crypt GGT5 5.016 0.00E+00 4.02E−01 5.03E−03 1.343247026 F.Crypt GNG11 3.200 0.00E+00 −8.10E−01  2.01E−23 1.5347982 F.Crypt GPX3 4.218 0.00E+00 5.13E−01 4.53E−11 2.829560076 F.Crypt GSN 3.608 0.00E+00 1.86E+00 0.00E+00 4.01570815 F.Crypt HAAO 3.538 0.00E+00 4.78E−01 1.81E−09 1.117489226 F.Crypt IFITM3 4.587 0.00E+00 1.81E+00  2.24E−305 4.693229283 F.Crypt IGFBP6 3.447 0.00E+00 2.88E−01 2.45E−03 1.802560823 F.Crypt IGFBP7 6.374 0.00E+00 2.12E+00  1.07E−150 6.278605 F.Crypt LAPTM4A 2.172  1.00E−225 1.15E+00  9.11E−216 1.650359625 F.Crypt LGALS1 4.361 0.00E+00 1.20E+00  2.63E−129 4.014277197 F.Crypt LINC01082 4.891 0.00E+00 3.90E−01 1.26E−03 1.832126089 F.Crypt LTBP4 2.845 0.00E+00 7.67E−01 5.61E−53 1.55451071 F.Crypt LUM 5.474 0.00E+00 2.63E+00  5.18E−131 4.610864086 F.Crypt MFAP4 5.218 0.00E+00 1.51E+00 8.79E−64 4.233927469 F.Crypt MFGE8 2.986 0.00E+00 −2.47E−01  1.09E−03 1.347363767 F.Crypt MMP2 3.597 0.00E+00 −2.95E−01  9.94E−05 1.902455796 F.Crypt MYL9 2.778 0.00E+00 −5.15E−01  1.34E−11 1.502286202 F.Crypt NGFRAP1 2.528 0.00E+00 6.10E−01 5.49E−56 1.354437953 F.Crypt NNMT 3.431 0.00E+00 −2.14E−01  1.54E−02 1.388286729 F.Crypt PCOLCE 3.816 0.00E+00 1.40E−01 1.41E−01 1.520934896 F.Crypt PLAC9 4.658 0.00E+00 3.18E−01 7.56E−03 2.119682525 F.Crypt PLAT 2.836 0.00E+00 −9.77E−01  1.02E−31 1.714357364 F.Crypt PLTP 3.245 0.00E+00 4.97E−01 2.42E−12 1.128031708 F.Crypt PMP22 3.549 0.00E+00 4.10E−01 5.72E−09 1.968640894 F.Crypt PPAP2A 2.665 0.00E+00 8.91E−01 1.70E−84 1.654665665 F.Crypt PPAP2B 4.323 0.00E+00 8.74E−01 8.59E−24 1.672913736 F.Crypt PPP1R14A 2.882 0.00E+00 3.39E−01 7.24E−09 2.075006444 F.Crypt PRKCDBP 3.358 0.00E+00 −1.01E−01  1.34E−01 1.868623908 F.Crypt PROCR 4.040 0.00E+00 6.40E−01 2.77E−18 2.45588358 F.Crypt PTGDS 4.801 0.00E+00 1.38E+00 3.35E−07 2.157176738 F.Crypt PTN 4.436 0.00E+00 4.86E−01 3.27E−05 1.90716397 F.Crypt RARRES2 3.704 0.00E+00 7.23E−01 1.11E−43 2.949004193 F.Crypt RBP1 4.222 0.00E+00 6.90E−01 1.61E−19 2.667468 F.Crypt S100A13 2.452  2.98E−301 5.56E−01 1.24E−40 1.18901627 F.Crypt SELM 2.910 0.00E+00 7.91E−01 8.90E−74 2.662116539 F.Crypt SEPPI 2.702 0.00E+00 8.41E−01 1.07E−55 2.690236454 F.Crypt SERPINF1 3.865 0.00E+00 3.20E−01 1.08E−05 2.625543209 F.Crypt SERPING1 3.525 0.00E+00 3.51E−01 1.15E−07 2.202321285 F.Crypt SGCE 3.394 0.00E+00 9.98E−02 1.93E−01 1.318068281 F.Crypt SOD3 4.535 0.00E+00 1.32E+00 1.26E−57 2.867761402 F.Crypt SPARC 3.291 0.00E+00 −2.81E−01  8.62E−05 2.178834875 F.Crypt SPARCL1 2.885 0.00E+00 −7.17E−01  2.83E−19 1.289030226 F.Crypt SPON2 3.311 0.00E+00 4.11E−01 2.88E−08 1.109871188 F.Crypt STMN2 4.214 0.00E+00 7.72E−01 9.69E−10 1.298791061 F.Crypt TCF21 5.007 0.00E+00 9.02E−01 3.64E−21 3.133263086 F.Crypt TIMP1 3.158 0.00E+00 8.42E−01 7.64E−62 3.071014624 F.Crypt TM4SF1 2.743 0.00E+00 1.77E−02 7.98E−01 1.620288745 F.Crypt TMEM176A 2.953 0.00E+00 1.16E+00  1.88E−195 2.275110559 F.Crypt TMEM176B 3.878 0.00E+00 1.81E+00 0.00E+00 4.09743926 F.Crypt TPM2 2.939 0.00E+00 −6.77E−01  5.60E−19 1.538165952 F.Crypt TSPAN4 3.028 0.00E+00 −1.37E−02  8.11E−01 1.529585907 F.Crypt VIM 3.222 0.00E+00 1.35E+00  8.69E−224 3.162898723 F.Crypt_hiFos A2M 4.512 0.00E+00 8.15E−01 3.22E−33 3.676893205 F.Crypt_hiFos ABCA8 4.194 0.00E+00 −4.76E−02  6.20E−01 2.649916107 F.Crypt_hiFos ADAMDEC1 7.088 0.00E+00 2.83E+00  4.26E−106 7.218882666 F.Crypt_hiFos APOE 6.567 0.00E+00 2.01E+00 3.43E−76 6.615669035 F.Crypt_hiFos C1R 5.565 0.00E+00 8.50E−01 2.64E−30 4.216039635 F.Crypt_hiFos C1S 5.634 0.00E+00 9.16E−01 5.97E−39 4.521134396 F.Crypt_hiFos CCL2 6.150 0.00E+00 1.27E+00 1.29E−30 5.123848379 F.Crypt_hiFos CCL8 4.875 0.00E+00 9.76E−01 3.13E−13 4.529100706 F.Crypt_hiFos CFD 6.860 0.00E+00 2.89E+00  9.60E−176 7.220630374 F.Crypt_hiFos COL1A1 4.013 0.00E+00 −1.52E−01  6.42E−02 2.82946601 F.Crypt_hiFos COL1A2 5.086 0.00E+00 2.94E−02 6.96E−01 3.494207311 F.Crypt_hiFos COL3A1 4.638 0.00E+00 1.50E−01 7.55E−02 3.596814435 F.Crypt_hiFos COL6A2 3.948 0.00E+00 −3.21E−01  2.07E−05 2.806908085 F.Crypt_hiFos CTSC 4.500  6.34E−256 1.89E+00  1.98E−199 4.569762818 F.Crypt_hiFos CXCL12 4.235 0.00E+00 3.80E−01 1.02E−06 3.1951176 F.Crypt_hiFos CXCL14 5.349  1.31E−258 2.52E+00  3.41E−138 5.763443334 F.Crypt_hiFos CYGB 4.188 0.00E+00 9.68E−02 1.58E−01 2.819846584 F.Crypt_hiFos DCN 6.287 0.00E+00 1.31E+00 1.48E−43 5.283090907 F.Crypt_hiFos FBLN1 5.461 0.00E+00 4.82E−01 5.93E−10 3.726786119 F.Crypt_hiFos GPX3 4.276 0.00E+00 2.55E−01 4.12E−04 3.3265932 F.Crypt_hiFos GSN 4.198  3.26E−202 1.61E+00  1.66E−141 4.426932662 F.Crypt_hiFos HAPLN1 4.502 0.00E+00 4.15E−01 2.32E−05 2.524390098 F.Crypt_hiFos IFITM3 4.767  2.69E−230 1.50E+00  3.30E−120 4.706261067 F.Crypt_hiFos IGFBP7 7.507 0.00E+00 1.40E+00 9.36E−43 6.303383638 F.Crypt_hiFos LUM 6.169 0.00E+00 1.29E+00 9.03E−34 5.351962011 F.Crypt_hiFos MFAP4 5.988 0.00E+00 7.99E−01 5.26E−23 4.555224313 F.Crypt_hiFos PPAP2B 3.920 0.00E+00 3.93E−01 9.26E−09 2.394203067 F.Crypt_hiFos PROCR 4.081 0.00E+00 2.87E−01 1.61E−05 3.077806433 F.Crypt_hiFos RBP1 4.194 0.00E+00 4.28E−01 5.10E−10 3.130240169 F.Crypt_hiFos SERPINF1 4.010 0.00E+00 4.87E−02 4.85E−01 3.045950154 F.Crypt_hiFos SOD3 4.488 0.00E+00 7.24E−01 1.16E−19 3.463482129 F.Crypt_hiFos TCF21 4.584 0.00E+00 2.38E−01 1.31E−03 3.283744234 F.Crypt_hiFos TMEM176B 4.410  7.82E−165 1.71E+00  1.08E−197 4.527681262 F.Crypt_hiFos VIM 4.984  3.19E−214 1.39E+00  1.13E−121 3.48544695 F.Crypt_loFos_1 A2M 4.566 0.00E+00 5.85E−01 2.88E−20 3.471644048 F.Crypt_loFos_1 ABCA8 4.248 0.00E+00 2.03E−01 4.13E−02 2.55026446 F.Crypt_loFos_1 ADAMDEC1 7.160 0.00E+00 3.05E+00  9.68E−134 6.568413627 F.Crypt_loFos_1 APOE 8.389 0.00E+00 2.58E+00  2.82E−151 7.136783921 F.Crypt_loFos_1 C1R 5.496 0.00E+00 7.93E−01 1.24E−30 4.131494165 F.Crypt_loFos_1 C1S 5.837 0.00E+00 6.91E−01 4.03E−22 4.237252058 F.Crypt_loFos_1 CALD1 4.220 0.00E+00 9.82E−03 8.86E−01 3.150459876 F.Crypt_loFos_1 CCL13 3.859 0.00E+00 7.60E−01 1.35E−04 3.58486718 F.Crypt_loFos_1 CCL2 4.141 0.00E+00 2.30E−01 4.37E−02 3.733752357 F.Crypt_loFos_1 CCL8 4.449 0.00E+00 2.59E−01 5.58E−02 3.576080936 F.Crypt_loFos_1 CFD 7.081 0.00E+00 3.01E+00  2.68E−209 7.152385774 F.Crypt_loFos_1 CFH 3.783 0.00E+00 1.85E−01 2.47E−02 2.220815228 F.Crypt_loFos_1 CLEC11A 3.494 0.00E+00 2.04E−01 4.21E−04 2.258975783 F.Crypt_loFos_1 COL1A1 4.014 0.00E+00 7.08E−02 3.52E−01 2.963298302 F.Crypt_loFos_1 COL1A2 5.242 0.00E+00 3.40E−01 2.62E−06 3.602018387 F.Crypt_loFos_1 COL3A1 4.942 0.00E+00 5.30E−01 7.50E−11 3.873803804 F.Crypt_loFos_1 COL6A2 3.984 0.00E+00 −2.72E−01  1.28E−04 2.837098282 F.Crypt_loFos_1 CTSC 4.685 0.00E+00 1.83E+00  1.10E−208 4.520244292 F.Crypt_loFos_1 CTSK 4.130 0.00E+00 2.49E−01 1.66E−03 2.620660286 F.Crypt_loFos_1 CXCL12 3.721 0.00E+00 3.29E−01 9.35E−05 2.775507108 F.Crypt_loFos_1 CXCL14 5.123 0.00E+00 2.51E+00  6.71E−163 5.704823079 F.Crypt_loFos_1 CYGB 4.375 0.00E+00 −5.80E−03  9.33E−01 2.860992966 F.Crypt_loFos_1 DCN 7.822 0.00E+00 1.52E+00 2.00E−63 5.238131885 F.Crypt_loFos_1 DKK3 3.769 0.00E+00 −2.18E−01  4.21E−03 1.908342802 F.Crypt_loFos_1 FBLN1 5.573 0.00E+00 3.66E−01 7.01E−06 3.461190649 F.Crypt_loFos_1 GGT5 3.900 0.00E+00 2.03E−01 9.92E−03 1.851084854 F.Crypt_loFos_1 GPX3 4.330 0.00E+00 4.80E−01 7.17E−13 3.458058087 F.Crypt_loFos_1 GSN 3.859  1.47E−254 1.60E+00  6.27E−159 4.263567086 F.Crypt_loFos_1 IFITM3 6.560 0.00E+00 1.77E+00  2.23E−192 5.166646778 F.Crypt_loFos_1 IGFBP7 7.514 0.00E+00 1.59E+00 6.62E−66 6.290186933 F.Crypt_loFos_1 LGALS1 5.430  1.44E−306 1.08E+00 1.33E−67 3.918497227 F.Crypt_loFos_1 LINC01082 4.011 0.00E+00 −2.52E−03  9.74E−01 2.466725414 F.Crypt_loFos_1 LUM 6.948 0.00E+00 1.46E+00 2.78E−44 5.224703375 F.Crypt_loFos_1 MFAP4 5.686 0.00E+00 9.07E−01 5.35E−29 4.455406471 F.Crypt_loFos_1 MMP2 3.547 0.00E+00 −3.40E−01  2.88E−07 2.36769262 F.Crypt_loFos_1 PLAC9 3.828 0.00E+00 1.85E−02 8.08E−01 2.327666003 F.Crypt_loFos_1 PMP22 3.692 0.00E+00 8.69E−02 2.23E−01 2.538680468 F.Crypt_loFos_1 PPAP2B 3.844 0.00E+00 3.25E−01 2.22E−06 2.317632739 F.Crypt_loFos_1 PROCR 4.373 0.00E+00 3.95E−01 6.81E−09 3.195637587 F.Crypt_loFos_1 PTN 3.804 0.00E+00 7.31E−02 3.62E−01 2.563456235 F.Crypt_loFos_1 RARRES2 3.874 0.00E+00 5.14E−01 2.99E−18 3.294341143 F.Crypt_loFos_1 RBP1 4.074 0.00E+00 3.93E−01 7.33E−10 3.101702956 F.Crypt_loFos_1 SERPINF1 3.726 0.00E+00 2.23E−01 6.29E−04 2.970864106 F.Crypt_loFos_1 SERPING1 3.431 0.00E+00 2.52E−01 4.68E−05 2.610215112 F.Crypt_loFos_1 SOD3 4.177 0.00E+00 7.64E−01 1.37E−23 3.282749538 F.Crypt_loFos_1 SPARC 3.802 0.00E+00 −1.66E−01  2.29E−02 2.730098195 F.Crypt_loFos_1 TCF21 4.897 0.00E+00 2.46E−01 9.84E−04 3.412667084 F.Crypt_loFos_1 TIMP1 4.084 0.00E+00 8.14E−01 5.04E−42 3.536639892 F.Crypt_loFos_1 TMEM176A 3.351  4.02E−211 1.10E+00  2.76E−128 2.998762433 F.Crypt_loFos_1 TMEM176B 4.864  8.48E−225 1.74E+00  1.12E−245 4.741101922 F.Crypt_loFos_1 VIM 5.295  5.46E−276 1.18E+00  1.88E−108 3.248254715 F.Crypt_loFos_2 APOE 5.899 0.00E+00 1.76E+00 1.67E−43 6.466993305 F.Crypt_loFos_2 CFD 5.299 0.00E+00 2.35E+00 3.36E−92 6.443773934 F.Endothelial BCAM 4.293 0.00E+00 1.23E+00 9.84E−42 1.212070381 F.Endothelial CAV1 4.086 0.00E+00 7.55E−01 1.03E−14 2.963859243 F.Endothelial CCDC85B 2.406  2.79E−184 1.30E+00  1.32E−165 1.989479948 F.Endothelial CD320 3.689 0.00E+00 3.25E+00 0.00E+00 3.29103572 F.Endothelial CD36 4.135 0.00E+00 1.90E+00 4.90E−39 2.182349023 F.Endothelial CD59 2.172  1.73E−130 1.53E+00  2.54E−236 1.506163126 F.Endothelial CLDN5 6.137 0.00E+00 3.07E+00 1.45E−25 3.338557396 F.Endothelial CLEC14A 5.319 0.00E+00 9.66E−01 3.87E−12 1.451043092 F.Endothelial CRIP2 4.642 0.00E+00 1.27E+00 2.67E−42 3.236897944 F.Endothelial EGFL7 6.013 0.00E+00 1.41E+00 5.14E−12 1.84382156 F.Endothelial ENG 3.721 0.00E+00 1.00E+00 3.27E−30 1.859620568 F.Endothelial ESAM 5.913 0.00E+00 1.59E+00 1.49E−18 1.438464574 F.Endothelial FABP5 3.117  1.32E−228 3.41E+00 0.00E+00 4.374347395 F.Endothelial FKBP1A 2.022  2.10E−112 1.50E+00  1.63E−264 1.788766568 F.Endothelial GIMAP7 3.221  1.42E−300 7.65E−01 2.55E−28 2.842038719 F.Endothelial GNG11 4.738 0.00E+00 1.85E+00  1.78E−120 4.14121094 F.Endothelial HLA-C 1.469 1.65E−11 1.59E+00 0.00E+00 2.645174636 F.Endothelial HLA-E 1.845 1.35E−74 1.66E+00 0.00E+00 2.607209735 F.Endothelial IFITM3 3.985  1.50E−298 1.75E+00  2.69E−201 4.533520832 F.Endothelial IGFBP4 3.576 0.00E+00 1.85E+00  8.00E−222 1.952179734 F.Endothelial IGFBP7 4.755 0.00E+00 1.67E+00 1.53E−71 5.974854235 F.Endothelial ITM2B 1.752 3.79E−56 1.97E+00 0.00E+00 2.756111513 F.Endothelial JAM2 5.981 0.00E+00 1.15E+00 3.42E−05 1.121967689 F.Endothelial MGP 4.392 0.00E+00 8.05E−01 8.10E−07 1.998657704 F.Endothelial NPDC1 3.004  3.12E−242 1.16E+00 6.47E−87 1.254551441 F.Endothelial PLVAP 6.365 0.00E+00 3.94E+00 8.19E−45 4.167360966 F.Endothelial RAMP2 5.270 0.00E+00 2.14E+00 8.66E−61 2.914625288 F.Endothelial RAMP3 8.188 0.00E+00 2.19E+00 5.51E−05 1.424899143 F.Endothelial RBP5 4.299 0.00E+00 5.14E−01 2.73E−05 1.573217657 F.Endothelial SEPW1 2.111  5.35E−106 1.47E+00  3.05E−269 2.044916625 F.Endothelial SLC9A3R2 3.082  2.77E−266 1.84E+00  1.69E−126 2.09792238 F.Endothelial SPARCL1 4.167 0.00E+00 1.32E+00 1.29E−55 3.33841819 F.Endothelial TM4SF1 3.406 0.00E+00 1.01E+00 7.43E−40 2.817273257 F.Endothelial TMEM88 5.627 0.00E+00 1.27E+00 3.57E−06 1.415444312 F.Endothelial VWF 8.023 0.00E+00 2.22E+00 2.29E−02 1.464896788 F.Endothelial_1 CD320 4.615  3.19E−220 3.53E+00 0.00E+00 4.954668807 F.Endothelial_1 CLDN5 5.988 0.00E+00 5.24E−01 1.28E−02 4.442027574 F.Endothelial_1 FABP5 4.513  1.86E−151 3.03E+00  2.87E−248 5.598134063 F.Endothelial_1 GNG11 4.944  2.31E−270 1.61E+00 5.47E−66 4.383616677 F.Endothelial_1 IGFBP4 3.758  3.71E−187 1.85E+00  3.16E−146 2.636215458 F.Endothelial_1 PLVAP 6.417 0.00E+00 1.88E+00 3.88E−21 5.305889624 F.Fibroblast A2M 3.869 0.00E+00 1.17E+00 1.10E−57 2.858008192 F.Fibroblast ADAMDEC1 3.583 0.00E+00 4.98E+00  1.90E−267 3.594023618 F.Fibroblast APOE 4.039 0.00E+00 3.22E+00  3.38E−168 4.921162902 F.Fibroblast BMP4 5.864 0.00E+00 1.00E+00 6.50E−07 1.42480642 F.Fibroblast C1R 5.580 0.00E+00 2.31E+00 7.05E−71 2.692699318 F.Fibroblast C1S 5.850 0.00E+00 2.13E+00 3.11E−49 2.913093084 F.Fibroblast CALD1 5.259 0.00E+00 6.73E−01 1.84E−07 2.814729165 F.Fibroblast CCL11 4.991 0.00E+00 2.97E+00 7.98E−08 1.681673822 F.Fibroblast CCL13 4.265 0.00E+00 3.42E+00 6.41E−26 1.449036254 F.Fibroblast CCL2 3.541 0.00E+00 1.41E+00 1.38E−22 2.112347447 F.Fibroblast CCL8 4.674 0.00E+00 2.67E+00 2.49E−26 1.387750615 F.Fibroblast CD63 2.229  2.01E−114 1.43E+00 0.00E+00 2.975250752 F.Fibroblast CFD 3.800 0.00E+00 4.03E+00  1.33E−289 4.028336506 F.Fibroblast CFH 5.163 0.00E+00 8.04E−01 2.06E−05 1.034054406 F.Fibroblast CLEC11A 4.337 0.00E+00 7.52E−01 1.23E−16 1.281757763 F.Fibroblast COL1A1 5.087 0.00E+00 1.51E+00 2.53E−25 2.075687041 F.Fibroblast COL1A2 5.820 0.00E+00 1.32E+00 1.22E−19 2.962132038 F.Fibroblast COL3A1 5.960 0.00E+00 2.06E+00 3.13E−30 2.867219098 F.Fibroblast COL6A1 4.892 0.00E+00 1.29E+00 1.08E−20 1.674302912 F.Fibroblast COL6A2 5.960 0.00E+00 1.49E+00 1.19E−17 2.844489178 F.Fibroblast CTSC 2.217  6.04E−280 1.78E+00  5.98E−242 2.19902085 F.Fibroblast CXCL12 4.276 0.00E+00 1.52E+00 1.55E−32 1.645919137 F.Fibroblast CXCL14 4.288 0.00E+00 4.13E+00 0.00E+00 5.862818394 F.Fibroblast CYGB 6.236 0.00E+00 1.22E+00 4.60E−12 1.721814926 F.Fibroblast DCN 5.155 0.00E+00 3.87E+00  3.97E−112 3.204355181 F.Fibroblast DMKN 3.898 0.00E+00 1.59E+00 1.34E−20 1.008034114 F.Fibroblast EID1 1.941  2.83E−209 9.60E−01  2.83E−165 1.465413201 F.Fibroblast EMILIN1 5.819 0.00E+00 1.04E+00 1.19E−07 1.055725268 F.Fibroblast FBLN1 6.416 0.00E+00 2.15E+00 1.21E−20 1.654953126 F.Fibroblast GNG11 2.966  3.60E−305 −1.21E+00  4.11E−46 1.064901305 F.Fibroblast GPX3 4.875 0.00E+00 1.03E+00 3.28E−22 2.355348742 F.Fibroblast GSN 2.553 0.00E+00 1.45E+00  9.12E−168 2.612701254 F.Fibroblast IFITM3 4.287 0.00E+00 1.91E+00 0.00E+00 4.209536056 F.Fibroblast IGFBP6 4.030 0.00E+00 4.48E−01 3.06E−04 1.420392445 F.Fibroblast IGFBP7 5.423 0.00E+00 1.92E+00 1.34E−86 5.704163002 F.Fibroblast LAMA4 4.389 0.00E+00 1.00E−01 4.76E−01 1.039331541 F.Fibroblast LAPTM4A 2.132  3.25E−223 1.30E+00  7.56E−280 1.339834069 F.Fibroblast LGALS1 4.316 0.00E+00 1.63E+00  7.62E−267 4.303949742 F.Fibroblast LGALS3BP 2.142  2.57E−224 1.08E+00  2.12E−204 1.091162389 F.Fibroblast LTBP4 3.130 0.00E+00 1.18E+00  5.17E−104 1.309909843 F.Fibroblast LUM 5.009 0.00E+00 3.79E+00 7.61E−97 2.964227078 F.Fibroblast MFAP4 6.497 0.00E+00 3.15E+00 4.74E−64 3.285006765 F.Fibroblast MFGE8 4.113 0.00E+00 9.42E−01 1.57E−13 1.289214426 F.Fibroblast MMP2 6.500 0.00E+00 1.66E+00 3.72E−12 1.747981548 F.Fibroblast MYL9 3.785 0.00E+00 4.76E−01 2.51E−04 1.942377438 F.Fibroblast NGFRAP1 2.546 0.00E+00 7.85E−01 3.46E−78 1.005472029 F.Fibroblast NNMT 4.284 0.00E+00 −6.65E−02  6.52E−01 1.043271273 F.Fibroblast PLAC9 5.422 0.00E+00 6.10E−01 6.25E−03 1.166274382 F.Fibroblast PLAT 3.585 0.00E+00 7.36E−01 4.31E−11 2.298300837 F.Fibroblast PMP22 3.499 0.00E+00 3.66E−01 2.39E−05 1.310460807 F.Fibroblast PPP1R14A 3.624 0.00E+00 8.61E−01 8.44E−31 2.050855445 F.Fibroblast PRKCDBP 3.972 0.00E+00 2.19E−01 2.86E−02 1.653768965 F.Fibroblast PROCR 5.144 0.00E+00 1.17E+00 2.40E−19 1.662380716 F.Fibroblast PTN 5.707 0.00E+00 5.65E−01 1.10E−02 1.06748513 F.Fibroblast RARRES2 4.164 0.00E+00 1.33E+00  4.13E−118 2.422426722 F.Fibroblast RBP1 4.610 0.00E+00 1.05E+00 1.54E−21 1.771585228 F.Fibroblast S100A13 2.664 0.00E+00 8.65E−01 3.26E−84 1.068941824 F.Fibroblast SDC2 4.548 0.00E+00 6.00E−01 2.34E−05 1.04905118 F.Fibroblast SELM 2.801 0.00E+00 1.18E+00  4.03E−158 2.474691328 F.Fibroblast SERPINF1 4.562 0.00E+00 1.04E+00 2.49E−24 2.265134228 F.Fibroblast SERPING1 3.893 0.00E+00 6.95E−01 1.18E−17 1.766270888 F.Fibroblast SOD3 4.119 0.00E+00 1.79E+00 1.53E−81 1.7043373 F.Fibroblast SPARC 3.920 0.00E+00 −5.69E−02  5.24E−01 2.258898195 F.Fibroblast TCF21 6.571 0.00E+00 1.33E+00 1.05E−10 1.816207729 F.Fibroblast TIMP1 3.012 0.00E+00 1.16E+00  1.19E−104 2.839662172 F.Fibroblast TM4SF1 3.104 0.00E+00 2.91E−01 8.34E−04 1.581472528 F.Fibroblast TMEM176A 2.830 0.00E+00 1.40E+00  1.16E−277 1.769196047 F.Fibroblast TMEM176B 3.791 0.00E+00 2.20E+00 0.00E+00 3.832911655 F.Fibroblast TPM2 4.664 0.00E+00 9.64E−01 4.00E−09 1.939714308 F.Fibroblast TSPAN4 3.186 0.00E+00 2.44E−01 2.05E−04 1.26975591 F.Fibroblast VIM 2.603 0.00E+00 1.23E+00  1.46E−198 2.867719694 F.Glia ALDH1A1 4.071  2.33E−198 2.62E+00  2.02E−201 3.761789138 F.Glia CD9 4.124  2.25E−110 2.31E+00  2.70E−220 4.789181961 F.Glia CLU 6.270 0.00E+00 2.13E+00 1.12E−48 5.703214125 F.Glia CRYAB 7.727 0.00E+00 3.82E+00  1.03E−142 6.612674122 F.Glia S100B 6.472 0.00E+00 2.20E+00 2.22E−23 4.64832577 F.Microvascular CD320 5.109  3.81E−136 3.11E+00  9.49E−225 5.155185625 F.Microvascular FABP5 5.789 1.22E−94 4.26E+00 0.00E+00 7.141626843 F.Microvascular PLVAP 8.376  5.02E−296 2.99E+00 2.61E−58 6.877072514 F.Myofibroblasts ACTA2 6.853  1.08E−258 3.42E+00  1.21E−118 6.872108933 F.Myofibroblasts TAGLN 6.260  1.93E−256 3.28E+00 2.29E−94 6.533966568 F.Stromal A2M 4.108 0.00E+00 1.73E+00 3.25E−93 2.420855705 F.Stromal ADAMDEC1 2.954 0.00E+00 4.68E+00  1.14E−198 2.910515351 F.Stromal APOE 2.975 0.00E+00 3.07E+00  1.74E−148 3.827897438 F.Stromal BMP4 5.111 0.00E+00 1.74E+00 3.18E−15 1.30003534 F.Stromal BST2 2.012  3.45E−242 9.82E−01  4.04E−122 1.935227746 F.Stromal C1R 5.080 0.00E+00 2.41E+00 1.09E−47 2.145519647 F.Stromal CIS 5.202 0.00E+00 2.60E+00 5.03E−47 2.33056005 F.Stromal CALD1 6.181 0.00E+00 1.95E+00 7.99E−15 1.966047523 F.Stromal CCL2 3.734 0.00E+00 2.05E+00 1.56E−30 1.986582677 F.Stromal CCL8 4.304 0.00E+00 2.83E+00 1.77E−24 1.144580585 F.Stromal CD63 1.819 1.79E−89 1.29E+00 0.00E+00 2.406521128 F.Stromal CFD 2.806 0.00E+00 4.00E+00  2.05E−268 2.868892416 F.Stromal CLEC11A 3.739 0.00E+00 9.36E−01 1.75E−24 1.025199717 F.Stromal COL1A1 5.431 0.00E+00 2.03E+00 7.75E−16 1.75794711 F.Stromal COL1A2 5.603 0.00E+00 2.25E+00 4.89E−26 2.478102984 F.Stromal COL3A1 5.196 0.00E+00 2.72E+00 2.58E−39 2.355722526 F.Stromal COL6A1 5.454 0.00E+00 1.47E+00 1.18E−09 1.375024981 F.Stromal COL6A2 5.503 0.00E+00 1.70E+00 9.14E−15 2.21250568 F.Stromal CTSC 1.583  3.43E−152 1.64E+00  1.13E−199 1.629643567 F.Stromal CXCL12 4.310 0.00E+00 1.60E+00 9.03E−26 1.242570645 F.Stromal CXCL14 2.342 0.00E+00 3.87E+00 0.00E+00 4.433021518 F.Stromal CYGB 5.565 0.00E+00 1.80E+00 1.20E−19 1.380616503 F.Stromal DCN 3.977 0.00E+00 3.86E+00  5.63E−126 2.624796179 F.Stromal EID1 1.833  2.53E−189 1.04E+00  1.08E−203 1.386022122 F.Stromal FBLN1 5.291 0.00E+00 2.51E+00 6.46E−23 1.542104205 F.Stromal GNG11 5.522 0.00E+00 2.03E+00 6.87E−16 1.024915045 F.Stromal GPX3 5.203 0.00E+00 2.14E+00 7.78E−41 1.908920129 F.Stromal GSN 2.806 0.00E+00 1.85E+00  1.20E−258 2.671887439 F.Stromal HSPB1 2.089  9.10E−212 1.13E+00  6.26E−190 1.97223964 F.Stromal IFITM1 2.098  3.42E−252 9.15E−01  3.94E−101 1.630880521 F.Stromal IFITM3 4.606 0.00E+00 2.62E+00 0.00E+00 4.057873527 F.Stromal IGFBP6 4.614 0.00E+00 1.46E+00 9.98E−16 1.209098122 F.Stromal IGFBP7 6.204 0.00E+00 4.58E+00 0.00E+00 5.88712189 F.Stromal LAPTM4A 2.041  3.57E−211 1.29E+00  5.86E−279 1.268032666 F.Stromal LGALS1 3.180 0.00E+00 1.70E+00  5.11E−250 4.001715701 F.Stromal LTBP4 2.655  1.13E−299 1.25E+00  5.14E−109 1.044916065 F.Stromal LUM 3.968 0.00E+00 3.64E+00 9.21E−91 2.418426911 F.Stromal MFAP4 4.998 0.00E+00 3.05E+00 1.99E−66 2.65491401 F.Stromal MMP2 6.151 0.00E+00 1.66E+00 1.03E−06 1.45210403 F.Stromal MYL9 4.791 0.00E+00 1.68E+00 1.22E−14 1.659548772 F.Stromal PLAT 4.548 0.00E+00 1.94E+00 1.74E−28 2.167799271 F.Stromal PMP22 3.820 0.00E+00 1.13E+00 6.81E−21 1.283005003 F.Stromal PPP1R14A 3.223 0.00E+00 1.01E+00 2.56E−39 1.700199238 F.Stromal PRKCDBP 5.658 0.00E+00 1.34E+00 3.79E−10 1.243717165 F.Stromal PROCR 4.810 0.00E+00 1.12E+00 6.77E−15 1.252978763 F.Stromal RARRES2 3.237 0.00E+00 1.40E+00  2.15E−110 1.838084217 F.Stromal RBP1 4.332 0.00E+00 1.30E+00 2.48E−27 1.423203449 F.Stromal SELM 2.476 0.00E+00 1.14E+00  4.80E−134 2.053452374 F.Stromal SERPINF1 3.472 0.00E+00 1.01E+00 1.47E−27 1.720141644 F.Stromal SERPING1 4.471 0.00E+00 1.20E+00 1.82E−26 1.455173755 F.Stromal SOD3 3.747 0.00E+00 2.28E+00 7.79E−96 1.301466108 F.Stromal SPARC 6.089 0.00E+00 2.11E+00 1.77E−23 2.08492746 F.Stromal SPARCL1 5.397 0.00E+00 2.19E+00 3.29E−18 1.157334608 F.Stromal TCF21 5.231 0.00E+00 1.98E+00 9.17E−25 1.514343398 F.Stromal TIMP1 2.749 0.00E+00 1.17E+00 1.48E−91 2.447949478 F.Stromal TM4SF1 3.823 0.00E+00 1.34E+00 1.41E−32 1.422652756 F.Stromal TMEM176A 1.962  3.88E−209 1.38E+00  9.94E−242 1.2868717 F.Stromal TMEM176B 2.318  1.97E−286 2.07E+00 0.00E+00 2.548034924 F.Stromal TPM2 4.510 0.00E+00 1.38E+00 1.36E−12 1.570324457 F.Stromal TSPAN4 3.521 0.00E+00 7.00E−01 8.16E−21 1.059144752 F.Stromal VIM 2.599 0.00E+00 1.27E+00  2.09E−203 2.963469114 F.Villus AGT 5.191 0.00E+00 7.61E−01 2.86E−03 1.565337446 F.Villus BMP4 4.133 0.00E+00 9.55E−01 3.23E−35 3.04641886 F.Villus C1S 3.052 0.00E+00 −6.76E−01  9.73E−21 2.265592255 F.Villus CALD1 3.626 0.00E+00 3.40E−01 8.31E−07 3.076513343 F.Villus CAV1 3.940 0.00E+00 3.44E−01 6.33E−04 2.679407949 F.Villus COL1A2 3.222 0.00E+00 −2.45E−01  7.00E−04 2.508175055 F.Villus COL3A1 3.337 0.00E+00 −3.69E−02  6.47E−01 2.699343963 F.Villus COL6A1 4.045 0.00E+00 9.09E−01 5.49E−33 3.105851972 F.Villus COL6A2 4.186 0.00E+00 8.33E−01 1.96E−28 3.587072611 F.Villus CXCL14 5.331 0.00E+00 3.87E+00 0.00E+00 6.639737212 F.Villus CYGB 3.575 0.00E+00 2.25E−01 6.46E−04 2.448508799 F.Villus DMKN 4.682 0.00E+00 1.76E+00 2.36E−49 3.100766685 F.Villus EDNRB 4.259 0.00E+00 6.52E−01 5.45E−10 1.964731755 F.Villus ENHO 5.765 0.00E+00 5.60E−01 5.06E−03 2.037996647 F.Villus F3 5.091 0.00E+00 1.41E+00 9.73E−25 2.111992756 F.Villus FRZB 4.758 0.00E+00 1.68E+00 4.91E−58 3.163962402 F.Villus GPX3 3.409 0.00E+00 2.34E−01 1.77E−04 2.723044038 F.Villus HSD17B2 2.813  2.90E−286 1.07E+00 4.46E−80 1.978660202 F.Villus IFITM3 3.410 0.00E+00 8.60E−01 6.14E−52 3.534780337 F.Villus IGFBP3 4.041 0.00E+00 1.30E+00 1.17E−25 2.513313933 F.Villus IGFBP7 4.072 0.00E+00 −3.70E−01  7.67E−05 4.395528895 F.Villus LGALS1 4.297 0.00E+00 1.49E+00  2.96E−146 4.260881439 F.Villus MFAP4 3.452 0.00E+00 −4.94E−01  6.77E−11 2.767660733 F.Villus MMP2 3.936 0.00E+00 7.39E−01 1.11E−27 3.105311214 F.Villus NBL1 2.298  8.07E−190 1.43E+00  2.84E−212 1.288462163 F.Villus NSG1 5.310 0.00E+00 1.17E+00 1.93E−16 2.688454505 F.Villus PLAT 4.548 0.00E+00 1.53E+00 4.34E−75 4.300004313 F.Villus POSTN 4.627 0.00E+00 1.79E+00 1.11E−35 3.366108575 F.Villus RARRES2 3.600 0.00E+00 9.47E−01 7.40E−62 3.155237799 F.Villus SDC2 3.610 0.00E+00 6.90E−01 1.47E−19 2.172949162 F.Villus SERPINF1 3.086 0.00E+00 3.73E−01 2.39E−08 2.484627191 F.Villus SPARC 3.176 0.00E+00 1.08E−01 1.27E−01 2.582445259 F.Villus TIMP1 2.751  2.30E−277 1.00E+00 1.07E−62 2.948613606 F.Villus TMEM176B 3.213  2.56E−272 1.64E+00  3.08E−240 3.649384031 F.Villus TPM2 3.507 0.00E+00 6.95E−01 1.29E−16 2.708057439 F.Villus VSTM2A 6.302 0.00E+00 1.17E+00 3.87E−05 1.94824354 F.Villus_1 CXCL14 5.215  1.74E−209 3.59E+00  4.77E−225 6.731692814 F.Villus_1 FRZB 4.374 0.00E+00 1.21E+00 1.92E−33 3.44591024 F.Villus_1 PLAT 4.344  2.06E−300 1.19E+00 6.68E−41 4.3838881 F.Villus_1 POSTN 4.774 0.00E+00 1.43E+00 4.92E−25 4.224144974 F.Villus_2 BMP4 4.055 0.00E+00 7.81E−01 1.46E−21 3.18144352 F.Villus_2 COL6A2 4.047 0.00E+00 7.36E−01 1.95E−22 3.663402198 F.Villus_2 CXCL14 5.188  1.56E−257 3.53E+00  1.21E−262 6.468476855 F.Villus_2 DMKN 4.194 0.00E+00 1.14E+00 1.96E−25 3.122402938 F.Villus_2 F3 4.600 0.00E+00 8.82E−01 1.40E−13 2.378018518 F.Villus_2 FRZB 4.341 0.00E+00 1.31E+00 1.27E−36 3.273271947 F.Villus_2 MMP2 3.863 0.00E+00 5.82E−01 1.14E−15 3.004724044 F.Villus_2 NSG1 4.447 0.00E+00 4.64E−01 1.67E−05 2.733631613 F.Villus_2 PLAT 4.234 0.00E+00 1.42E+00 9.20E−57 4.328991007 F.Villus_2 RARRES2 3.647  4.28E−284 9.70E−01 4.92E−50 3.333240445 I.Immune ARHGDIB 4.207 0.00E+00 7.82E−01 6.32E−22 3.181654331 I.Immune CCL5 3.713 0.00E+00 2.86E+00 5.61E−41 3.227650679 I.Immune CD37 5.394 0.00E+00 2.57E−01 2.73E−01 1.385527254 I.Immune CD3D 4.743 0.00E+00 1.63E+00 1.37E−11 2.656028184 I.Immune CD3E 5.114 0.00E+00 1.25E+00 4.63E−06 2.008260655 I.Immune CD52 5.341 0.00E+00 1.58E+00 2.86E−13 3.098900803 I.Immune CD69 3.468 0.00E+00 9.81E−01 7.45E−15 2.209932935 I.Immune CD7 4.101 0.00E+00 2.28E+00 1.90E−27 1.902035143 I.Immune CORO1A 5.181 0.00E+00 1.37E+00 1.40E−16 2.294753907 I.Immune CST3 −3.303 0.00E+00 5.57E−01 1.48E−17 −2.400189989 I.Immune CYBA 1.716  1.86E−131 1.11E+00  2.74E−244 1.660237626 I.Immune EVL 3.462 0.00E+00 6.54E−01 2.05E−11 1.493950621 I.Immune HCST 5.437 0.00E+00 7.94E−01 6.19E−04 1.609957297 I.Immune LAPTM5 5.136 0.00E+00 8.70E−01 3.17E−05 1.184622899 I.Immune LTB 4.541 0.00E+00 1.46E+00 5.87E−07 1.551222258 I.Immune PTPRCAP 5.120 0.00E+00 1.23E+00 1.08E−11 2.166023611 I.Immune RAC2 4.648 0.00E+00 6.56E−01 5.34E−07 1.313198 I.Immune RGS1 3.798 0.00E+00 1.15E+00 3.62E−22 2.015574355 I.Immune SRGN 3.581 0.00E+00 3.14E−01 1.61E−04 2.825816153 I.Immune TRBC2 4.401 0.00E+00 1.45E+00 5.26E−12 2.825938206 I.Lymphoid ARHGDIB 3.161 0.00E+00 2.32E−01 4.47E−05 3.051707434 I.Lymphoid CCL5 4.003 0.00E+00 2.91E+00 4.01E−44 3.723272334 I.Lymphoid CD2 4.995 0.00E+00 7.92E−01 5.47E−03 2.213341168 I.Lymphoid CD3D 4.827 0.00E+00 1.84E+00 1.44E−17 3.248239337 I.Lymphoid CD3E 5.611 0.00E+00 1.26E+00 2.42E−05 2.497000932 I.Lymphoid CD52 3.726 0.00E+00 1.10E+00 2.79E−32 3.478443808 I.Lymphoid CD69 2.848 0.00E+00 5.09E−02 5.93E−01 2.43959911 I.Lymphoid CD7 4.040 0.00E+00 2.42E+00 1.15E−39 2.231958553 I.Lymphoid CORO1A 3.316 0.00E+00 7.40E−01 7.28E−22 2.580002303 I.Lymphoid CYTIP 3.486 0.00E+00 2.17E−01 1.62E−02 1.083215597 I.Lymphoid EVL 3.009  2.49E−308 8.04E−01 1.35E−25 1.719868351 I.Lymphoid IL32 1.886  7.28E−217 1.53E+00  1.65E−150 2.754297032 I.Lymphoid LTB 3.458 0.00E+00 1.22E+00 6.33E−15 1.960757541 I.Lymphoid PTPRCAP 5.483 0.00E+00 9.99E−01 1.59E−11 2.664468478 I.Lymphoid RAC2 3.576 0.00E+00 4.91E−01 2.55E−09 1.619586858 I.Lymphoid TRAC 3.277 0.00E+00 9.75E−01 4.22E−23 2.970592688 I.Lymphoid TRBC2 4.628 0.00E+00 1.31E+00 8.72E−12 3.495017388 M.CD69pos Mast H3F3B 3.540 1.14E−70 2.04E+00 0.00E+00 4.709127236 M.CD69pos Mast NFKBIA 2.588  4.21E−135 2.26E+00  3.68E−261 3.816864413 M.CD69pos Mast PPP1R15A 2.241  4.32E−119 1.88E+00  3.12E−235 2.716247642 M.CD69pos Mast TPSAB1 8.102 0.00E+00 5.34E+00 1.96E−81 8.759937866 M.CD69pos Mast VWA5A 4.147  4.01E−306 2.24E+00  2.67E−153 2.804667246 M.DCs AIF1 5.554 0.00E+00 6.91E−02 5.32E−01 4.109607894 M.DCs CD74 6.686  1.89E−172 4.31E+00 0.00E+00 7.361182144 M.DCs CPVL 5.451 0.00E+00 9.74E−01 1.72E−13 3.259858496 M.DCs CST3 5.077 1.81E−84 3.22E+00 0.00E+00 6.239191066 M.DCs HLA-DMA 5.034 0.00E+00 1.19E+00 1.06E−60 3.949279865 M.DCs HLA-DMB 4.713 0.00E+00 2.68E−02 7.46E−01 2.996355003 M.DCs HLA-DPA1 7.499 0.00E+00 3.16E+00  3.81E−219 6.620670842 M.DCs HLA-DPB1 7.613 0.00E+00 3.30E+00  1.84E−212 7.191760426 M.DCs HLA-DQA1 7.085 0.00E+00 1.57E+00 3.77E−47 5.548948208 M.DCs HLA-DQB1 6.326 0.00E+00 1.65E+00 9.64E−76 4.944199971 M.DCs HLA-DRA 7.705 0.00E+00 3.77E+00  2.22E−196 7.875311998 M.DCs HLA-DRB1 7.430  4.72E−272 3.62E+00  5.06E−285 7.13770053 M.DCs HLA-DRB5 4.876 0.00E+00 1.85E+00 3.04E−68 4.910951864 M.DCs LST1 5.039 0.00E+00 2.99E−01 1.74E−03 3.486090838 M.DCs LYZ 5.747 0.00E+00 2.04E+00 1.56E−44 5.88694392 M.Macrophages ACP5 3.187  4.27E−303 1.34E+00 6.76E−73 2.590818222 M.Macrophages AIF1 5.576 0.00E+00 1.04E+00 1.07E−22 4.307976358 M.Macrophages C1QA 6.150 0.00E+00 2.87E+00 1.46E−84 5.300031996 M.Macrophages C1QB 6.052 0.00E+00 2.86E+00 7.25E−75 4.677009635 M.Macrophages C1QC 6.172 0.00E+00 2.57E+00 1.21E−69 4.762331438 M.Macrophages CD74 5.009  7.44E−287 3.39E+00 0.00E+00 6.179449074 M.Macrophages CST3 3.100  2.80E−150 2.47E+00 0.00E+00 4.680553349 M.Macrophages CTSB 2.952  8.47E−251 1.92E+00  7.20E−294 2.192366953 M.Macrophages CTSD 2.222  5.30E−145 1.99E+00 0.00E+00 2.293098548 M.Macrophages CTSZ 2.801  8.27E−225 1.20E+00  1.03E−124 1.283964758 M.Macrophages CYBA 1.691 7.98E−52 1.72E+00 0.00E+00 2.742799342 M.Macrophages DNASE1L3 5.106 0.00E+00 9.20E−01 3.60E−09 2.994302955 M.Macrophages FCER1G 4.663 0.00E+00 9.35E−01 2.28E−28 4.105822052 M.Macrophages FCGRT 2.078  1.29E−112 1.35E+00  1.21E−221 1.42923146 M.Macrophages FTL 4.189 2.32E−26 4.10E+00 0.00E+00 6.501041387 M.Macrophages FUCA1 2.678  3.03E−209 1.80E+00  1.44E−157 1.444883944 M.Macrophages GPX1 3.408  1.48E−239 2.08E+00 0.00E+00 3.660866748 M.Macrophages HLA-DMA 3.705 0.00E+00 1.27E+00 2.39E−89 2.908577367 M.Macrophages HLA-DMB 3.933 0.00E+00 8.50E−01 4.73E−26 2.265503073 M.Macrophages HLA-DPA1 4.231 0.00E+00 2.53E+00  1.04E−207 5.115407151 M.Macrophages HLA-DPB1 5.213 0.00E+00 2.35E+00  5.56E−166 5.724454744 M.Macrophages HLA-DQA1 4.701 0.00E+00 1.18E+00 3.01E−30 4.031618355 M.Macrophages HLA-DQB1 3.829 0.00E+00 9.39E−01 1.29E−31 3.050844971 M.Macrophages HLA-DRA 5.837 0.00E+00 2.84E+00  4.85E−170 6.499764955 M.Macrophages HLA-DRB1 5.097 0.00E+00 2.83E+00  1.57E−257 5.910780843 M.Macrophages HLA-DRB5 3.390 0.00E+00 1.74E+00 1.88E−77 3.498438452 M.Macrophages IGSF6 5.196 0.00E+00 5.53E−01 2.67E−04 1.625886678 M.Macrophages LGMN 2.996  7.35E−263 1.72E+00  2.49E−165 1.837166624 M.Macrophages LST1 4.287 0.00E+00 −1.14E−01  2.10E−01 2.582366499 M.Macrophages LYZ 4.983 0.00E+00 1.99E+00 1.85E−41 4.35619307 M.Macrophages MS4A4A 5.392 0.00E+00 7.67E−01 3.65E−05 1.044712017 M.Macrophages MS4A6A 5.055 0.00E+00 8.89E−01 1.94E−13 2.624760555 M.Macrophages MS4A7 5.211 0.00E+00 7.97E−01 2.20E−07 1.824855194 M.Macrophages NPC2 2.844  1.41E−177 2.19E+00 0.00E+00 2.979535936 M.Macrophages PSAP 2.931  2.19E−193 2.40E+00 0.00E+00 3.379791933 M.Macrophages RNASE1 2.869  2.01E−246 2.02E+00  4.73E−141 2.33910545 M.Macrophages RNASET2 2.002  5.77E−127 1.47E+00  1.81E−255 1.746194062 M.Macrophages S100A11 2.110  1.58E−119 1.51E+00  1.50E−219 2.530747738 M.Macrophages SAT1 3.003  8.08E−149 2.35E+00 0.00E+00 4.071450542 M.Macrophages SEPP1 2.949  9.84E−254 1.64E+00  5.90E−136 3.60554335 M.Macrophages STAB1 5.244 0.00E+00 4.85E−01 3.14E−03 1.299766554 M.Macrophages TMSB4X 3.375 2.03E−05 2.11E+00 0.00E+00 2.573438479 M.Macrophages TYROBP 5.234 0.00E+00 1.63E+00 7.88E−86 4.732860448 M.Mast CAPG 2.432  4.98E−146 1.70E+00  6.15E−192 2.17915183 M.Mast H3F3B 3.313 3.21E−65 1.93E+00 0.00E+00 4.47755371 M.Mast NFKBIA 2.271  1.45E−118 2.20E+00  2.86E−255 3.455658808 M.Mast PPP1R15A 2.033  2.06E−108 1.87E+00  1.26E−240 2.476327326 M.Mast TPSAB1 8.512 0.00E+00 6.42E+00  4.45E−163 8.639427859 M.Mast VWA5A 4.283 0.00E+00 2.45E+00  7.39E−197 2.846401762 M.Monocytes ACP5 2.724  8.51E−303 9.53E−01 3.39E−33 1.882241762 M.Monocytes AIF1 6.739 0.00E+00 2.17E+00 9.08E−46 4.232871977 M.Monocytes AMICA1 3.065 0.00E+00 8.74E−02 2.31E−01 1.677961646 M.Monocytes C1QA 5.492 0.00E+00 4.03E+00 2.99E−69 4.155816971 M.Monocytes C1QB 5.282 0.00E+00 3.70E+00 7.83E−53 3.441937672 M.Monocytes C1QC 5.400 0.00E+00 3.19E+00 9.69E−45 3.642706749 M.Monocytes C1orf162 3.733 0.00E+00 −1.04E−01  2.85E−01 1.170437832 M.Monocytes CD74 5.291 0.00E+00 3.98E+00 0.00E+00 6.598762611 M.Monocytes COTL1 2.597  7.05E−307 9.03E−01 5.44E−85 2.212565365 M.Monocytes CPVL 5.896 0.00E+00 1.33E+00 3.40E−11 1.189459222 M.Monocytes CST3 3.513  6.58E−239 2.90E+00 0.00E+00 5.233170493 M.Monocytes CTSB 2.202  2.93E−211 1.55E+00  9.60E−204 1.356719163 M.Monocytes CYBA 1.897 2.10E−81 1.50E+00 0.00E+00 2.769627973 M.Monocytes DNASE1L3 6.099 0.00E+00 2.45E+00 9.24E−18 2.563358103 M.Monocytes FAM26F 4.957 0.00E+00 2.28E−01 1.99E−01 1.145484272 M.Monocytes FCER1G 4.804 0.00E+00 7.06E−01 9.51E−13 3.864097586 M.Monocytes FGL2 3.941 0.00E+00 9.35E−01 4.92E−21 1.291638448 M.Monocytes FTL 3.690 6.14E−25 3.33E+00 0.00E+00 5.135226719 M.Monocytes GPX1 3.523 0.00E+00 1.94E+00 0.00E+00 3.477841098 M.Monocytes HLA-DMA 4.277 0.00E+00 1.60E+00  7.42E−148 3.137660058 M.Monocytes HLA-DMB 4.587 0.00E+00 8.74E−01 1.14E−22 2.298238533 M.Monocytes HLA-DPA1 4.926 0.00E+00 3.06E+00 0.00E+00 5.55420434 M.Monocytes HLA-DPB1 5.650 0.00E+00 3.21E+00 0.00E+00 6.141157002 M.Monocytes HLA-DQA1 5.332 0.00E+00 2.21E+00 8.84E−99 4.355634178 M.Monocytes HLA-DQA2 3.920 0.00E+00 8.37E−01 3.45E−10 1.7733194 M.Monocytes HLA-DQB1 4.715 0.00E+00 1.86E+00  4.05E−100 3.47409069 M.Monocytes HLA-DQB2 4.951 0.00E+00 3.95E−01 2.47E−02 1.429331185 M.Monocytes HLA-DRA 6.364 0.00E+00 3.77E+00 0.00E+00 6.90336385 M.Monocytes HLA-DRB1 5.624 0.00E+00 3.53E+00 0.00E+00 6.291170635 M.Monocytes HLA-DRB5 4.212 0.00E+00 2.13E+00  2.24E−103 3.906936969 M.Monocytes IL1B 5.314 0.00E+00 2.02E+00 1.23E−09 1.362160979 M.Monocytes ITGB2 3.243 0.00E+00 1.26E−01 7.84E−02 1.46825593 M.Monocytes LAPTM5 2.698 0.00E+00 1.33E−01 1.19E−02 2.055128002 M.Monocytes LGALS1 3.002 0.00E+00 8.09E−01 9.54E−44 3.344243506 M.Monocytes LST1 5.286 0.00E+00 6.40E−01 1.30E−07 2.821686152 M.Monocytes LYZ 5.942 0.00E+00 3.45E+00 2.44E−87 4.680781408 M.Monocytes MS4A6A 6.354 0.00E+00 1.78E+00 9.88E−17 2.246168647 M.Monocytes MS4A7 5.854 0.00E+00 1.02E+00 6.74E−05 1.332493787 M.Monocytes NPC2 2.814  2.22E−246 1.78E+00 0.00E+00 2.574957856 M.Monocytes PLAUR 2.657  3.67E−283 1.12E+00 3.46E−56 1.648644174 M.Monocytes PSAP 2.534  5.30E−224 1.91E+00 0.00E+00 2.503500359 M.Monocytes RGS10 2.565 0.00E+00 4.82E−01 4.78E−31 2.150189084 M.Monocytes RNASE6 4.098 0.00E+00 9.94E−01 4.50E−21 1.036740582 M.Monocytes RNASET2 2.270  2.04E−218 1.30E+00  6.18E−257 1.751116723 M.Monocytes S100A11 2.204  3.20E−179 1.28E+00  2.47E−222 2.369494044 M.Monocytes SAT1 3.237  2.41E−232 2.09E+00 0.00E+00 3.959712325 M.Monocytes SPI1 4.890 0.00E+00 1.01E+00 2.42E−17 1.592825824 M.Monocytes TMSB4X 3.136 8.25E−06 2.05E+00 0.00E+00 2.614405699 M.Monocytes TYMP 2.489  3.09E−282 9.52E−01  2.47E−101 1.861697922 M.Monocytes TYROBP 5.333 0.00E+00 1.66E+00 1.01E−62 4.513467018 M.Myeloid AIF1 5.813 0.00E+00 2.02E+00 1.09E−33 2.305919495 M.Myeloid C1QA 4.690 0.00E+00 3.98E+00 1.50E−84 2.293597851 M.Myeloid C1QB 4.688 0.00E+00 4.01E+00 5.78E−68 1.93454735 M.Myeloid C1QC 5.203 0.00E+00 3.75E+00 2.68E−46 1.994680241 M.Myeloid CD74 1.729  2.70E−174 3.83E+00 0.00E+00 3.96445085 M.Myeloid CST3 1.583  1.20E−114 2.55E+00 0.00E+00 2.496545122 M.Myeloid CYBA 0.845 3.74E−30 1.30E+00 0.00E+00 1.355375364 M.Myeloid DNASE1L3 5.938 0.00E+00 2.54E+00 5.07E−17 1.357649186 M.Myeloid FCER1G 5.155 0.00E+00 7.53E−01 6.05E−10 3.351878581 M.Myeloid FTH1 2.972 6.58E−17 1.58E+00 0.00E+00 3.161764242 M.Myeloid FTL 3.481 2.47E−46 2.81E+00 0.00E+00 5.143530637 M.Myeloid GLUL 2.625  9.29E−308 1.05E+00 2.08E−81 1.104516091 M.Myeloid GPX1 2.294  7.45E−245 1.92E+00 0.00E+00 1.892173705 M.Myeloid HLA-DMA 3.140 0.00E+00 1.61E+00  8.42E−166 1.804731204 M.Myeloid HLA-DMB 4.269 0.00E+00 1.05E+00 1.83E−26 1.310971013 M.Myeloid HLA-DPA1 2.822 0.00E+00 3.07E+00 0.00E+00 3.603351858 M.Myeloid HLA-DPB1 3.000 0.00E+00 3.42E+00 0.00E+00 3.960321522 M.Myeloid HLA-DQA1 4.043 0.00E+00 2.04E+00 1.83E−73 2.645131811 M.Myeloid HLA-DQA2 3.981 0.00E+00 7.23E−01 8.78E−06 1.096108771 M.Myeloid HLA-DQB1 3.588 0.00E+00 1.90E+00  8.14E−107 2.070477499 M.Myeloid HLA-DRA 3.065 0.00E+00 3.69E+00 0.00E+00 4.339804481 M.Myeloid HLA-DRB1 2.879 0.00E+00 3.40E+00 0.00E+00 3.753125817 M.Myeloid HLA-DRB5 3.170 0.00E+00 2.12E+00  1.23E−103 2.390321388 M.Myeloid LST1 4.767 0.00E+00 4.39E−01 7.52E−04 1.650785876 M.Myeloid LYZ 4.702 0.00E+00 3.68E+00  7.62E−110 2.556327471 M.Myeloid MS4A6A 6.737 0.00E+00 1.99E+00 1.24E−17 1.009965999 M.Myeloid NPC2 2.140  6.05E−205 1.71E+00 0.00E+00 1.557639793 M.Myeloid PSAP 1.917  4.55E−178 1.82E+00 0.00E+00 1.557168286 M.Myeloid S100A11 1.592  1.63E−131 1.21E+00  1.01E−219 1.623417727 M.Myeloid SAT1 1.885  4.03E−151 2.00E+00 0.00E+00 2.378322556 M.Myeloid SRGN 2.346  3.11E−303 6.68E−01 2.24E−51 2.663800303 M.Myeloid TMSB4X 3.924 1.08E−11 1.61E+00 0.00E+00 2.455257638 M.Myeloid TYROBP 4.999 0.00E+00 1.22E+00 2.51E−22 3.317457944 M.Tissue_DCs AIF1 5.733 0.00E+00 3.04E−01 6.77E−03 4.343902986 M.Tissue_DCs CD74 6.537  8.69E−147 4.22E+00 0.00E+00 7.317250586 M.Tissue_DCs CLEC10A 5.783 0.00E+00 1.04E+00 4.56E−13 3.638767911 M.Tissue_DCs CST3 4.913 7.85E−72 3.17E+00 0.00E+00 6.099017935 M.Tissue_DCs HLA-DMA 5.111  5.40E−280 1.36E+00 1.87E−71 4.010642012 M.Tissue_DCs HLA-DPA1 7.274  3.20E−256 3.23E+00  2.20E−206 6.561614831 M.Tissue_DCs HLA-DPB1 7.476  3.55E−290 3.09E+00  4.68E−164 7.139900132 M.Tissue_DCs HLA-DQA1 6.883 0.00E+00 1.65E+00 1.64E−46 5.545865153 M.Tissue_DCs HLA-DQB1 6.394 0.00E+00 1.75E+00 1.37E−75 4.964711147 M.Tissue_DCs HLA-DRA 7.540  1.52E−267 3.88E+00  3.58E−183 7.91753476 M.Tissue_DCs HLA-DRB1 7.352  5.21E−243 3.50E+00  5.44E−237 7.1857139 M.Tissue_DCs LST1 5.239 0.00E+00 4.97E−01 7.18E−08 3.72542232 M.Tissue_DCs LYZ 5.579 0.00E+00 2.14E+00 3.62E−44 5.80083893 T.CD4 ARHGDIB 2.714 0.00E+00 6.95E−01 5.09E−60 2.948999621 T.CD4 B2M 2.524 4.10E−11 1.31E+00 0.00E+00 3.181207891 T.CD4 BTG1 2.081  8.64E−201 1.29E+00  3.42E−241 2.666942355 T.CD4 CD2 3.325 0.00E+00 −4.30E−02  5.70E−01 2.361888134 T.CD4 CD3D 3.865 0.00E+00 −1.53E−01  3.12E−02 3.285517157 T.CD4 CD3E 3.298 0.00E+00 −1.03E−01  9.38E−02 2.441937608 T.CD4 CD52 3.093 0.00E+00 4.27E−01 6.58E−15 3.285206277 T.CD4 EEF1A1 1.811 1.44E−18 1.29E+00 0.00E+00 2.913519854 T.CD4 IL32 3.257 0.00E+00 9.29E−01 7.35E−73 3.875940105 T.CD4 LTB 3.303 0.00E+00 5.68E−01 2.19E−11 2.960038975 T.CD4 RPL10 1.878 5.33E−17 1.19E+00 0.00E+00 2.933302608 T.CD4 RPL21 2.075 2.43E−43 1.20E+00 0.00E+00 3.077829574 T.CD4 RPLP1 2.061 3.31E−25 1.22E+00 0.00E+00 2.97564638 T.CD4 RPS19 2.122 1.71E−40 1.24E+00 0.00E+00 3.029170811 T.CD4 RPS25 1.749 4.46E−50 1.10E+00 0.00E+00 2.510200315 T.CD4 RPS27 1.969 2.14E−30 1.29E+00 0.00E+00 3.052783949 T.CD4 RPS27A 1.880 5.73E−50 1.22E+00 0.00E+00 2.910333285 T.CD4 RPS3 1.822 1.75E−33 1.14E+00 0.00E+00 2.909904991 T.CD4 TMEM66 1.634  1.36E−148 9.77E−01  2.12E−191 1.516743632 T.CD4 TMSB4X 2.596 3.91E−08 1.50E+00 0.00E+00 2.234471623 T.CD4 TRAC 3.572 0.00E+00 6.66E−01 7.52E−26 3.57637506 T.CD4 TRBC2 3.692 0.00E+00 4.12E−01 1.65E−08 3.684828708 T.CD8 ACTB 2.475 3.60E−42 1.50E+00 0.00E+00 3.50971244 T.CD8 ARHGDIB 2.865 0.00E+00 6.08E−01 1.44E−49 2.982840619 T.CD8 B2M 3.216 1.13E−08 1.43E+00 0.00E+00 2.404427044 T.CD8 CCL5 5.160 0.00E+00 2.00E+00  4.92E−151 5.905248855 T.CD8 CD3D 3.462 0.00E+00 4.53E−01 6.24E−15 3.394691814 T.CD8 CD3E 3.001 0.00E+00 2.17E−01 1.56E−05 2.761361085 T.CD8 CD52 3.267 0.00E+00 7.59E−01 2.58E−46 3.532187537 T.CD8 CD7 3.358 0.00E+00 9.13E−01 2.79E−31 3.042456161 T.CD8 CORO1A 2.680 0.00E+00 6.16E−01 3.12E−38 2.743977822 T.CD8 EVL 2.487  2.00E−302 5.33E−01 1.11E−29 2.184459445 T.CD8 GZMA 3.738 0.00E+00 1.48E+00 1.48E−21 3.352055654 T.CD8 HCST 2.860 0.00E+00 5.95E−01 1.90E−34 2.695248321 T.CD8 HOPX 3.414 0.00E+00 5.97E−01 1.12E−13 2.402446002 T.CD8 IL32 3.922 0.00E+00 1.20E+00  3.71E−150 4.279234249 T.CD8 NKG7 4.290 0.00E+00 6.17E−01 7.86E−08 3.272826393 T.CD8 PTPRCAP 2.633 0.00E+00 8.49E−01 1.44E−69 2.810217158 T.CD8 SH3BGRL3 1.886  5.60E−118 1.05E+00  5.36E−212 2.458584789 T.CD8 TMSB4X 4.143 4.19E−11 1.88E+00 0.00E+00 2.661426524 T.CD8 TRAC 2.825 0.00E+00 2.81E−01 2.77E−07 3.041416989 T.CD8 TRBC2 3.074 0.00E+00 1.88E−01 1.58E−03 3.233102921 T.CD8_IELs CCL5 6.114 0.00E+00 1.88E+00  2.57E−123 6.194585882 T.CD8_IELs CD3D 3.256 0.00E+00 5.35E−01 1.20E−18 3.441592568 T.CD8_IELs CD52 3.451  1.72E−306 7.40E−01 1.11E−37 3.498103129 T.CD8_IELs CD7 3.988 0.00E+00 1.24E+00 4.14E−68 4.046757488 T.CD8_IELs HOPX 3.762 0.00E+00 5.68E−01 3.21E−13 3.314436098 T.CD8_IELs IL32 4.020  2.09E−271 1.38E+00  4.88E−124 4.322274876 T.CD8_IELs NKG7 3.841 0.00E+00 −3.01E−02  7.46E−01 3.446184383 T.CD8 LP CCL5 5.676 0.00E+00 1.27E+00 5.56E−57 5.633700535 T.CD8 LP NKG7 3.722 0.00E+00 4.11E−01 3.52E−05 3.486023674 T.Tcells ACTB 2.020 4.86E−40 1.65E+00 0.00E+00 3.316981313 T.Tcells ARHGDIB 3.191 0.00E+00 1.10E+00  3.46E−131 3.341126137 T.Tcells B2M 2.272 1.17E−09 1.50E+00 0.00E+00 3.065937757 T.Tcells BTG1 1.763  8.44E−157 1.26E+00  2.58E−229 2.123789859 T.Tcells CCL5 4.279 0.00E+00 2.74E+00 1.64E−83 4.302419639 T.Tcells CD2 5.172 0.00E+00 6.17E−01 7.82E−05 2.052746914 T.Tcells CD3D 6.166 0.00E+00 2.08E+00 5.91E−46 3.397618572 T.Tcells CD3E 6.421 0.00E+00 7.92E−01 4.38E−07 2.370389625 T.Tcells CD52 4.108 0.00E+00 1.20E+00 1.58E−68 3.95478922 T.Tcells CD7 4.693 0.00E+00 9.36E−01 1.78E−11 2.221062807 T.Tcells CKLF 2.025  3.39E−207 1.20E+00  2.90E−176 1.080775129 T.Tcells CORO1A 3.262 0.00E+00 1.09E+00 7.57E−77 2.860991596 T.Tcells EVL 3.434 0.00E+00 9.82E−01 1.41E−49 2.035932542 T.Tcells GZMA 3.945 0.00E+00 2.12E+00 1.82E−18 1.960681705 T.Tcells HCST 3.243 0.00E+00 7.05E−01 4.60E−27 2.173769075 T.Tcells HOPX 4.032 0.00E+00 6.86E−01 5.98E−07 1.726884514 T.Tcells IL2RG 2.193  7.47E−228 1.17E+00  1.41E−136 1.152000617 T.Tcells IL32 4.161 0.00E+00 1.81E+00  8.41E−260 4.656688606 T.Tcells LCK 4.921 0.00E+00 6.42E−01 8.05E−07 1.507134026 T.Tcells LTB 3.053 0.00E+00 3.90E−01 3.13E−04 2.116429025 T.Tcells MYL12A 1.681  2.24E−123 1.06E+00  3.94E−231 1.746942368 T.Tcells NKG7 4.103 0.00E+00 2.56E−01 1.48E−01 1.791038239 T.Tcells PTPRCAP 3.216 0.00E+00 1.41E+00  4.57E−128 2.773769069 T.Tcells RAC2 2.651 0.00E+00 1.13E+00 2.04E−99 1.676182044 T.Tcells RPLP1 1.843 1.24E−20 1.12E+00 0.00E+00 2.762677204 T.Tcells RPS19 2.379 6.55E−43 1.34E+00 0.00E+00 3.222843513 T.Tcells RPS27 2.047 1.14E−31 1.22E+00 0.00E+00 3.079388618 T.Tcells RPS27A 1.878 5.06E−50 1.19E+00 0.00E+00 2.82253802 T.Tcells SH3BGRL3 1.894  7.78E−139 1.22E+00  1.42E−266 2.177941405 T.Tcells TMEM66 1.554  3.21E−135 1.03E+00  2.83E−211 1.23170526 T.Tcells TMSB4X 3.485 6.22E−17 2.01E+00 0.00E+00 3.017818451 T.Tcells TRAC 4.649 0.00E+00 1.34E+00 9.50E−47 3.593010994 T.Tcells TRBC2 5.165 0.00E+00 1.21E+00 3.55E−24 3.838266308 ident pvalH n ref_n mu ref_mu total ref_total B.Bcells 0 2578 359 5.641 2.160 0.988 0.012 B.Bcells 0 2871 54 3.440 2.038 0.993 0.007 B.Bcells 0 2822 654 2.141 3.245 0.667 0.333 B.Bcells 0 4698 3412 6.225 5.422 0.706 0.294 B.Bcells 0 4236 96 3.539 2.601 0.988 0.012 B.Bcells 0 3975 6433 3.404 4.208 0.261 0.739 B.Bcells 0 2866 202 3.310 1.484 0.980 0.020 B.Bcells 0 2886 1147 2.490 2.410 0.727 0.273 B.Bcells 0 2838 1234 3.073 2.136 0.815 0.185 B.Bcells 0 4045 2898 4.309 2.510 0.829 0.171 B.Bcells 0 4090 3927 10.531 4.627 0.984 0.016 B.Bcells 0 3316 1856 8.718 3.178 0.988 0.012 B.Bcells 0 3809 2394 8.956 3.375 0.987 0.013 B.Bcells 0 4051 2015 9.672 3.306 0.994 0.006 B.Bcells 0 3141 970 9.006 2.698 0.996 0.004 B.Bcells 0 3104 1057 8.945 2.694 0.996 0.004 B.Bcells 0 3236 327 4.523 2.282 0.979 0.021 B.Bcells 0 3514 1633 3.061 3.806 0.562 0.438 B.Bcells 0 3115 1862 3.082 2.014 0.778 0.222 B.FO 0 1636 3662 7.169 5.408 0.602 0.398 B.FO 0 1329 611 4.069 3.148 0.805 0.195 B.FO 0 1424 1964 6.368 5.807 0.517 0.483 B.Plasma 0 1938 476 5.757 3.326 0.956 0.044 B.Plasma 0 1952 187 3.086 3.582 0.881 0.119 B.Plasma 0 1446 67 1.049 1.739 0.930 0.070 B.Plasma 0 1965 694 1.883 3.067 0.555 0.445 B.Plasma 0 2232 415 2.837 3.768 0.738 0.262 B.Plasma 0 2047 1483 1.669 1.866 0.546 0.454 B.Plasma 0 1614 1080 0.998 2.928 0.282 0.718 B.Plasma 0 2257 308 3.404 2.046 0.949 0.051 B.Plasma 0 2175 1211 2.502 2.401 0.658 0.342 B.Plasma 0 1575 464 1.118 2.147 0.625 0.375 B.Plasma 0 1896 390 1.327 2.039 0.748 0.252 B.Plasma 0 1938 2367 1.332 3.351 0.168 0.832 B.Plasma 0 1464 743 0.806 2.612 0.360 0.640 B.Plasma 0 1743 692 0.998 1.926 0.570 0.430 B.Plasma 0 987 57 0.872 1.673 0.909 0.091 B.Plasma 0 2264 1310 3.132 2.155 0.773 0.227 B.Plasma 0 1711 310 0.885 1.806 0.745 0.255 B.Plasma 0 1812 1347 1.099 2.730 0.303 0.697 B.Plasma 0 2289 2972 4.600 2.649 0.749 0.251 B.Plasma 0 2277 3971 11.091 6.041 0.950 0.050 B.Plasma 0 2191 1943 9.110 4.205 0.971 0.029 B.Plasma 0 2276 2508 9.345 5.235 0.940 0.060 B.Plasma 0 2236 2285 10.236 5.820 0.954 0.046 B.Plasma 0 2004 1122 9.451 5.412 0.967 0.033 B.Plasma 0 1949 1188 9.318 5.456 0.960 0.040 B.Plasma 0 1489 229 7.071 4.038 0.982 0.018 B.Plasma 0 1665 1897 0.949 2.751 0.201 0.799 B.Plasma 0 2132 1910 1.991 2.682 0.409 0.591 B.Plasma 0 2167 1989 2.174 2.088 0.536 0.464 B.Plasma 0 2288 444 4.708 3.157 0.938 0.062 B.Plasma 0 1847 1542 1.330 2.140 0.406 0.594 B.Plasma 0 1994 1742 1.575 1.818 0.492 0.508 B.Plasma 0 1754 530 1.437 2.396 0.630 0.370 B.Plasma 0 1913 1076 1.259 1.678 0.571 0.429 B.Plasma 0 2173 1824 2.321 2.002 0.598 0.402 B.Plasma 0 1876 1532 2.366 4.316 0.241 0.759 B.Plasma 0 1935 1939 3.018 4.263 0.296 0.704 B.Plasma 0 2188 2170 2.399 2.306 0.518 0.482 B.Plasma 0 2257 1916 3.186 2.059 0.720 0.280 B.Plasma 0 1997 1374 1.537 1.815 0.545 0.455 B.Plasma 0 2186 2124 2.197 2.042 0.534 0.466 B.Plasma 0 2304 4597 5.264 3.048 0.700 0.300 B.Plasma 0 2144 159 2.368 2.270 0.935 0.065 B.Plasma 0 2074 1697 1.437 2.029 0.448 0.552 B.Plasma 0 1851 906 1.197 1.820 0.570 0.430 B.Plasma 0 2142 1136 1.859 1.783 0.665 0.335 B.Plasma 0 1182 181 3.150 2.281 0.923 0.077 B.Plasma 0 2269 2366 3.808 2.402 0.718 0.282 E.Absorptive 0 2419 1210 5.657 4.012 0.862 0.138 E.Absorptive 0 2368 1676 4.134 3.090 0.744 0.256 E.Absorptive 0 2543 2453 3.920 3.230 0.626 0.374 E.Absorptive 0 2538 2572 4.215 3.389 0.636 0.364 E.Absorptive 0 2569 2856 4.828 4.237 0.575 0.425 E.Absorptive 0 2586 3229 7.343 6.378 0.610 0.390 E.Absorptive 0 2636 7360 8.704 6.761 0.579 0.421 E.Absorptive 0 2604 2999 5.836 4.833 0.635 0.365 E.Absorptive 0 2291 1543 6.851 4.898 0.852 0.148 E.Absorptive 0 1915 864 6.005 3.687 0.917 0.083 E.Absorptive 0 2319 1549 3.931 3.630 0.648 0.352 E.Absorptive 0 2625 3403 5.557 5.034 0.526 0.474 E.Absorptive 0 2615 4913 5.677 4.600 0.529 0.471 E.Absorptive 0 2255 1042 4.595 3.340 0.838 0.162 E.Absorptive 0 2629 3625 7.680 6.559 0.612 0.388 E.Absorptive 0 2235 1712 4.390 3.443 0.716 0.284 E.Absorptive 0 2413 1313 3.557 2.644 0.776 0.224 E.Absorptive 0 2552 3904 4.571 3.259 0.619 0.381 E.Absorptive 0 2510 2308 4.466 3.800 0.633 0.367 E.Absorptive_All 0 6268 2463 4.694 3.733 0.832 0.168 E.Absorptive_All 0 5395 1757 3.378 2.208 0.874 0.126 E.Absorptive_All 0 5581 1642 4.383 2.304 0.935 0.065 E.Absorptive_All 0 5855 2149 3.753 2.912 0.830 0.170 E.Absorptive_All 0 6196 2409 4.475 3.788 0.805 0.195 E.Absorptive_All 0 5203 2380 3.467 2.281 0.833 0.167 E.Absorptive_All 0 6288 2771 7.262 4.198 0.950 0.050 E.Absorptive_All 0 6280 2556 5.411 4.074 0.861 0.139 E.Absorptive_All 0 5846 2079 4.970 3.024 0.915 0.085 E.Absorptive_All 0 6520 2928 5.497 4.207 0.845 0.155 E.Absorptive_All 0 6456 4467 5.441 3.867 0.811 0.189 E.Absorptive_All 0 6540 2740 5.707 4.974 0.799 0.201 E.Absorptive_All 0 6653 3203 7.396 5.409 0.892 0.108 E.Absorptive_All 0 6008 2284 5.037 3.789 0.862 0.138 E.Absorptive_All 0 4148 778 2.897 2.025 0.907 0.093 E.Absorptive_All 0 4088 681 4.251 1.773 0.971 0.029 E.Absorptive_All 0 5736 3566 3.994 2.566 0.812 0.188 E.Absorptive_All 0 5391 1861 3.459 2.234 0.871 0.129 E.Absorptive_All 0 5464 1809 4.071 2.982 0.865 0.135 E.Absorptive_TA_1 0 1888 3219 5.228 5.469 0.332 0.668 E.Best4_Enterocytes 0 883 79 4.152 1.316 0.988 0.012 E.Best4_Enterocytes 0 1008 159 4.234 2.208 0.963 0.037 E.Best4_Enterocytes 0 998 312 2.542 2.166 0.806 0.194 E.Enterocyte_Immature_1 0 1208 986 3.636 2.657 0.707 0.293 E.Enterocyte_Immature_1 0 1509 1055 6.138 4.740 0.790 0.210 E.Enterocyte_Immature_1 0 1448 2202 3.934 2.974 0.561 0.439 E.Enterocyte_Immature_1 0 1541 1211 5.270 4.437 0.694 0.306 E.Enterocyte_Immature_1 0 1469 1685 4.045 3.252 0.602 0.398 E.Enterocyte_Immature_1 0 1355 926 3.502 3.047 0.667 0.333 E.Enterocyte_Immature_1 0 1160 562 3.641 2.825 0.784 0.216 E.Enterocyte_Immature_1 0 1245 791 3.305 2.625 0.716 0.284 E.Enterocyte_Immature_1 0 1649 3213 7.297 6.450 0.480 0.520 E.Enterocyte_Immature_1 0 1624 2958 5.587 4.929 0.464 0.536 E.Enterocyte_Immature_1 0 1576 1563 6.327 5.274 0.677 0.323 E.Enterocyte_Immature_1 0 1375 869 4.845 4.491 0.669 0.331 E.Enterocyte_Immature_1 0 1397 1101 4.274 3.659 0.660 0.340 E.Enterocyte_Immature_1 0 1636 7064 9.382 7.272 0.500 0.500 E.Enterocyte_Immature_1 0 1650 3582 7.715 6.569 0.505 0.495 E.Enterocyte_Immature_1 0 1508 1743 4.271 3.450 0.604 0.396 E.Enterocyte_Immature_1 0 1303 988 3.838 2.743 0.738 0.262 E.Enterocyte_Immature_1 0 1364 1389 3.484 2.750 0.620 0.380 E.Enterocyte_Immature_1 0 1511 1278 4.441 3.959 0.623 0.377 E.Enterocyte_Immature_1 0 1585 2292 4.562 3.771 0.545 0.455 E.Enterocyte_Immature_2 0 1613 1448 5.329 4.259 0.700 0.300 E.Enterocyte_Immature_2 0 1733 2294 4.949 3.991 0.595 0.405 E.Enterocyte_Immature_2 0 1706 2741 4.217 2.898 0.608 0.392 E.Enterocyte_Immature_2 0 1742 3229 8.185 6.228 0.677 0.323 E.Enterocyte_Immature_2 0 1741 2988 6.218 4.786 0.611 0.389 E.Enterocyte_Immature_2 0 1728 2665 5.773 4.442 0.620 0.380 E.Enterocyte_Immature_2 0 1686 1570 4.051 3.624 0.591 0.409 E.Enterocyte_Immature_2 0 1740 3405 6.253 4.952 0.557 0.443 E.Enterocyte_Immature_2 0 1739 4853 6.280 4.541 0.545 0.455 E.Enterocyte_Immature_2 0 1651 1026 3.644 3.194 0.687 0.313 E.Enterocyte_Immature_2 0 1742 3640 8.382 6.389 0.656 0.344 E.Enterocyte_Immature_2 0 1657 1239 3.473 2.556 0.716 0.284 E.Enterocyte_Immature_2 0 1681 1257 4.082 3.996 0.587 0.413 E.Enterocyte_Immature_2 0 1563 722 2.284 2.256 0.688 0.312 E.Enterocyte_Immature_2 0 1721 2289 4.045 3.026 0.604 0.396 E.Enterocyte_Progenitor 0 1449 1447 5.583 4.128 0.733 0.267 E.Enterocyte_Progenitor 0 1666 2312 5.128 3.860 0.634 0.366 E.Enterocyte_Progenitor 0 1775 3197 7.585 6.413 0.556 0.444 E.Enterocyte_Progenitor 0 1750 2962 5.506 4.937 0.467 0.533 E.Enterocyte_Progenitor 0 1732 2698 5.418 4.421 0.562 0.438 E.Enterocyte_Progenitor 0 1788 3407 5.829 4.994 0.483 0.517 E.Enterocyte_Progenitor 0 1794 3248 6.231 5.312 0.511 0.489 E.Enterocyte_Progenitor 0 1805 3625 7.738 6.539 0.533 0.467 E.Enterocyte_Progenitor 0 1571 2085 4.310 2.747 0.690 0.310 E.Enterocytes 0 1208 975 3.631 2.639 0.711 0.289 E.Enterocytes 0 917 355 1.979 1.221 0.814 0.186 E.Enterocytes 0 1300 1081 6.579 4.568 0.829 0.171 E.Enterocytes 0 1399 2198 4.012 2.940 0.572 0.428 E.Enterocytes 0 1373 1236 5.591 4.360 0.723 0.277 E.Enterocytes 0 1332 890 3.427 2.674 0.716 0.284 E.Enterocytes 0 1401 1679 4.545 3.150 0.687 0.313 E.Enterocytes 0 1365 915 3.753 2.942 0.724 0.276 E.Enterocytes 0 1357 1984 3.033 2.101 0.566 0.434 E.Enterocytes 0 1246 523 3.893 2.827 0.833 0.167 E.Enterocytes 0 1138 521 2.204 1.612 0.767 0.233 E.Enterocytes 0 1400 2545 4.586 3.458 0.546 0.454 E.Enterocytes 0 1287 769 3.495 2.429 0.778 0.222 E.Enterocytes 0 1163 628 2.203 2.004 0.680 0.320 E.Enterocytes 0 1407 7359 9.255 6.746 0.521 0.479 E.Enterocytes 0 1406 2957 6.072 4.857 0.525 0.475 E.Enterocytes 0 1245 840 2.147 1.559 0.690 0.310 E.Enterocytes 0 1360 1569 6.764 5.134 0.728 0.272 E.Enterocytes 0 1323 842 5.194 4.497 0.718 0.282 E.Enterocytes 0 1312 1210 3.191 2.445 0.645 0.355 E.Enterocytes 0 1273 867 2.494 2.449 0.602 0.398 E.Enterocytes 0 1407 3535 6.492 4.715 0.577 0.423 E.Enterocytes 0 1396 3426 4.999 4.657 0.341 0.659 E.Enterocytes 0 1370 1546 3.900 3.754 0.495 0.505 E.Enterocytes 0 1329 1109 4.750 3.508 0.739 0.261 E.Enterocytes 0 1367 1283 2.746 2.110 0.623 0.377 E.Enterocytes 0 1296 1000 3.998 3.267 0.683 0.317 E.Enterocytes 0 1269 765 2.116 1.954 0.650 0.350 E.Enterocytes 0 1004 338 1.924 1.388 0.812 0.188 E.Enterocytes 0 1318 1256 3.092 2.264 0.651 0.349 E.Enterocytes 0 1400 1769 4.877 3.398 0.688 0.312 E.Enterocytes 0 1271 976 3.950 2.808 0.742 0.258 E.Enterocytes 0 1269 906 2.510 2.150 0.643 0.357 E.Enterocytes 0 1383 1375 3.797 2.739 0.677 0.323 E.Enterocytes 0 1361 1268 5.029 3.857 0.708 0.292 E.Enterocytes 0 1252 769 2.441 2.197 0.659 0.341 E.Enterocytes 0 1396 3893 4.751 3.276 0.499 0.501 E.Enterocytes 0 1189 699 2.159 1.498 0.729 0.271 E.Enterocytes 0 1282 561 2.649 2.497 0.718 0.282 E.Enterocytes 0 1405 2295 4.950 3.765 0.582 0.418 E.Epithelial 0 5973 612 4.662 2.328 0.980 0.020 E.Epithelial 0 307 3272 3.229 4.267 0.044 0.956 E.Epithelial 0 3989 5281 1.787 4.098 0.132 0.868 E.Epithelial 0 6692 739 4.464 2.690 0.969 0.031 E.Epithelial 0 5641 162 3.091 1.879 0.988 0.012 E.Epithelial 0 5315 529 4.057 2.477 0.968 0.032 E.Epithelial 0 5479 542 4.053 2.368 0.970 0.030 E.Epithelial 0 6025 324 3.331 2.067 0.978 0.022 E.Epithelial 0 5725 313 3.030 1.789 0.977 0.023 E.Epithelial 0 6329 341 3.514 2.357 0.976 0.024 E.Epithelial 0 6657 3899 3.928 2.819 0.787 0.213 E.Epithelial 0 2953 4393 1.575 4.053 0.108 0.892 E.Epithelial 0 6291 7064 3.410 4.852 0.247 0.753 E.Epithelial 0 5939 220 2.986 1.950 0.982 0.018 E.Epithelial 0 6749 538 4.356 2.299 0.981 0.019 E.Epithelial 0 6503 1475 6.761 2.996 0.984 0.016 E.Epithelial 0 4839 273 4.634 2.143 0.990 0.010 E.Epithelial 0 6836 736 5.030 2.380 0.983 0.017 E.Epithelial 0 6115 6812 3.156 4.678 0.238 0.762 E.Epithelial 0 4232 77 2.454 2.392 0.983 0.017 E.Epithelial 0 6506 1536 4.979 4.205 0.879 0.121 E.Epithelial 0 1130 3867 1.024 3.483 0.050 0.950 E.Epithelial 0 4787 5723 2.296 4.826 0.127 0.873 E.Epithelial 0 6932 773 4.516 2.208 0.978 0.022 E.Epithelial 0 6214 504 4.638 2.285 0.984 0.016 E.Epithelial 0 3967 188 3.602 2.227 0.982 0.018 E.Epithelial 0 7212 1063 5.228 2.254 0.982 0.018 E.Epithelial 0 536 4026 1.750 4.763 0.016 0.984 E.Epithelial 0 6974 3280 5.112 3.428 0.872 0.128 E.Epithelial 0 7167 943 5.524 2.568 0.983 0.017 E.Epithelial 0 6851 6095 6.555 4.769 0.795 0.205 E.Epithelial 0 6938 6665 6.706 4.903 0.784 0.216 E.Epithelial 0 6912 5562 6.655 5.153 0.779 0.221 E.Epithelial 0 4403 256 3.945 2.516 0.979 0.021 E.Epithelial 0 6432 562 4.723 2.396 0.983 0.017 E.Epithelial 0 6606 7339 4.757 5.640 0.328 0.672 E.Epithelial 0 7408 5397 6.193 4.281 0.838 0.162 E.Epithelial 0 6127 139 3.183 2.235 0.988 0.012 E.Epithelial 0 5976 1086 2.970 2.252 0.900 0.100 E.Epithelial 0 5745 240 3.827 2.062 0.988 0.012 E.Epithelial 0 3260 4585 1.622 4.032 0.118 0.882 E.Goblet 0 1014 1738 4.280 3.261 0.542 0.458 E.Goblet 0 1028 2386 4.238 2.967 0.510 0.490 E.Goblet 0 1019 2318 3.786 2.986 0.434 0.566 E.Goblet 0 1130 1888 6.958 3.952 0.828 0.172 E.Goblet 0 1139 2993 5.805 4.876 0.420 0.580 E.Goblet 0 1116 2845 5.250 3.470 0.574 0.426 E.Goblet 0 1144 3565 5.970 4.780 0.423 0.577 E.Goblet 0 1013 1161 4.358 3.537 0.606 0.394 E.Goblet 0 901 980 3.415 1.838 0.733 0.267 E.Goblet 0 1147 1035 6.701 3.303 0.921 0.079 E.Goblet 0 1047 874 5.978 3.644 0.858 0.142 E.Goblet 0 1155 2699 8.105 6.062 0.638 0.362 E.Goblet 0 1112 2295 4.690 3.832 0.468 0.532 E.Goblet 0 1152 1799 9.543 5.487 0.914 0.086 E.Immature_Enterocytes 0 2770 974 5.397 4.780 0.814 0.186 E.Immature_Enterocytes 0 4103 2842 4.682 4.247 0.661 0.339 E.Immature_Enterocytes 0 3737 2024 3.594 2.779 0.765 0.235 E.Immature_Enterocytes 0 3209 1234 5.279 3.343 0.909 0.091 E.Immature_Enterocytes 0 3984 2104 4.839 3.403 0.837 0.163 E.Immature_Enterocytes 0 3148 1205 2.557 1.970 0.797 0.203 E.Immature_Enterocytes 0 2795 702 3.278 2.891 0.839 0.161 E.Immature_Enterocytes 0 3495 2259 4.787 3.428 0.799 0.201 E.Immature_Enterocytes 0 3987 2429 3.904 3.355 0.706 0.294 E.Immature_Enterocytes 0 2467 682 2.970 2.406 0.842 0.158 E.Immature_Enterocytes 0 4002 2792 4.364 4.240 0.610 0.390 E.Immature_Enterocytes 0 3518 2703 3.810 2.732 0.733 0.267 E.Immature_Enterocytes 0 4306 3066 7.752 5.616 0.861 0.139 E.Immature_Enterocytes 0 4259 2804 5.786 4.542 0.783 0.217 E.Immature_Enterocytes 0 3313 1399 5.742 5.195 0.776 0.224 E.Immature_Enterocytes 0 4043 3078 4.457 4.346 0.586 0.414 E.Immature_Enterocytes 0 3925 2492 5.394 3.918 0.814 0.186 E.Immature_Enterocytes 0 3478 1272 3.920 3.183 0.820 0.180 E.Immature_Enterocytes 0 4298 3250 5.891 4.632 0.760 0.240 E.Immature_Enterocytes 0 4231 4762 5.744 4.378 0.696 0.304 E.Immature_Enterocytes 0 4267 3099 5.988 5.204 0.703 0.297 E.Immature_Enterocytes 0 3067 767 3.589 2.881 0.867 0.133 E.Immature_Enterocytes 0 4339 3536 7.965 5.941 0.833 0.167 E.Immature_Enterocytes 0 3955 2610 4.983 4.291 0.710 0.290 E.Immature_Enterocytes 0 3423 1503 3.872 3.325 0.769 0.231 E.Immature_Enterocytes 0 2621 844 3.295 2.782 0.816 0.184 E.Immature_Enterocytes 0 3107 1191 2.956 2.634 0.765 0.235 E.Immature_Enterocytes 0 3242 1926 3.977 2.504 0.824 0.176 E.Immature_Enterocytes 0 3097 1082 3.413 2.109 0.876 0.124 E.Immature_Enterocytes 0 3549 972 4.198 3.576 0.849 0.151 E.Immature_Enterocytes 0 2613 579 2.414 1.908 0.865 0.135 E.Immature_Enterocytes 0 3743 2268 3.484 2.977 0.701 0.299 E.Immature_Enterocytes 0 3919 3787 4.221 3.085 0.695 0.305 E.Immature_Enterocytes 0 3721 2131 3.735 2.740 0.777 0.223 E.Immature_Enterocytes 0 3931 2068 4.145 3.590 0.736 0.264 E.Immature_Goblet 0 1551 2662 5.765 4.313 0.615 0.385 E.Immature_Goblet 0 1359 695 5.136 2.744 0.911 0.089 E.Immature_Goblet 0 1573 1880 5.942 4.318 0.720 0.280 E.Immature_Goblet 0 1565 966 5.946 3.560 0.894 0.106 E.Immature_Goblet 0 1530 954 4.467 2.127 0.890 0.110 E.Immature_Goblet 0 1605 3182 4.941 4.379 0.427 0.573 E.Immature_Goblet 0 1175 381 2.500 0.954 0.900 0.100 E.Immature_Goblet 0 1480 1003 4.504 4.612 0.578 0.422 E.Immature_Goblet 0 1191 439 2.826 1.954 0.832 0.168 E.Immature_Goblet 0 1193 409 4.378 1.993 0.938 0.062 E.Immature_Goblet 0 1408 1494 3.866 3.130 0.611 0.389 E.Immature_Goblet 0 1224 828 3.130 2.242 0.732 0.268 E.Immature_Goblet 0 1382 1364 3.880 2.933 0.661 0.339 E.Immature_Goblet 0 1236 768 6.140 4.371 0.846 0.154 E.Immature_Goblet 0 1658 2739 8.816 5.512 0.857 0.143 E.Immature_Goblet 0 1370 959 4.276 2.274 0.851 0.149 E.Immature_Goblet 0 1449 1816 7.937 6.485 0.686 0.314 E.Secretory 0 1291 1951 6.784 3.914 0.829 0.171 E.Secretory 0 1845 3181 5.589 4.243 0.596 0.404 E.Secretory 0 1231 1080 6.606 3.313 0.918 0.082 E.Secretory 0 1131 920 5.885 3.694 0.849 0.151 E.Secretory 0 1794 2690 7.582 6.100 0.651 0.349 E.Secretory 0 1349 1854 9.323 5.425 0.916 0.084 E.Secretory_All 0 2517 603 4.459 1.756 0.965 0.035 E.Secretory_All 0 3656 1746 5.947 2.828 0.948 0.052 E.Secretory_All 0 3924 2945 4.548 5.087 0.478 0.522 E.Secretory_All 0 3044 802 5.231 2.741 0.955 0.045 E.Secretory_All 0 3200 755 3.709 1.530 0.950 0.050 E.Secretory_All 0 4218 3113 5.026 4.144 0.714 0.286 E.Secretory_All 0 4234 3340 4.732 5.151 0.487 0.513 E.Secretory_All 0 4111 3186 5.379 5.488 0.545 0.455 E.Secretory_All 0 3391 817 5.311 1.951 0.977 0.023 E.Secretory_All 0 2389 240 2.570 0.913 0.969 0.031 E.Secretory_All 0 2326 612 5.647 3.504 0.944 0.056 E.Secretory_All 0 4234 2580 8.009 4.159 0.959 0.041 E.Secretory_All 0 3449 1682 8.247 3.561 0.981 0.019 E.Tuft 0 552 3208 6.765 4.217 0.502 0.498 F.Crypt 0 3156 920 4.099 3.199 0.865 0.135 F.Crypt 0 2386 78 3.398 2.781 0.979 0.021 F.Crypt 0 1779 316 2.763 1.870 0.913 0.087 F.Crypt 0 3497 556 7.247 3.992 0.984 0.016 F.Crypt 0 2123 327 3.330 1.894 0.946 0.054 F.Crypt 0 3623 868 7.043 5.086 0.942 0.058 F.Crypt 0 2087 487 2.812 3.595 0.713 0.287 F.Crypt 0 3308 639 4.365 3.670 0.893 0.107 F.Crypt 0 3341 614 4.536 3.693 0.907 0.093 F.Crypt 0 2951 718 3.608 3.828 0.779 0.221 F.Crypt 0 2221 119 5.921 3.852 0.987 0.013 F.Crypt 0 1919 48 5.837 2.060 0.998 0.002 F.Crypt 0 2986 445 4.944 4.651 0.892 0.108 F.Crypt 0 2149 64 5.018 1.983 0.996 0.004 F.Crypt 0 3624 5585 5.307 4.208 0.582 0.418 F.Crypt 0 3596 926 6.711 3.192 0.978 0.022 F.Crypt 0 2375 360 3.327 2.554 0.919 0.081 F.Crypt 0 2375 500 2.948 2.424 0.872 0.128 F.Crypt 0 2949 618 3.768 3.722 0.831 0.169 F.Crypt 0 3310 671 4.189 3.910 0.857 0.143 F.Crypt 0 3281 671 4.522 4.262 0.854 0.146 F.Crypt 0 2324 591 3.038 3.498 0.741 0.259 F.Crypt 0 3069 706 3.715 3.901 0.793 0.207 F.Crypt 0 3322 2236 4.673 2.996 0.826 0.174 F.Crypt 0 2564 397 3.253 2.783 0.899 0.101 F.Crypt 0 2503 333 3.720 2.966 0.927 0.073 F.Crypt 0 3542 2197 6.261 5.187 0.772 0.228 F.Crypt 0 2782 488 3.451 3.339 0.860 0.140 F.Crypt 0 3546 596 5.853 4.297 0.946 0.054 F.Crypt 0 1979 213 2.670 3.009 0.880 0.120 F.Crypt 0 1732 188 3.131 2.839 0.919 0.081 F.Crypt 0 1789 319 2.403 2.658 0.825 0.175 F.Crypt 0 2102 375 2.752 2.686 0.854 0.146 F.Crypt 0 1146 42 3.718 3.221 0.975 0.025 F.Crypt 0 3283 344 4.242 2.792 0.963 0.037 F.Crypt 0 1902 156 2.727 2.171 0.947 0.053 F.Crypt 0 2145 630 2.846 3.905 0.620 0.380 F.Crypt 0 2755 567 3.695 3.335 0.862 0.138 F.Crypt 0 3351 2620 4.812 3.347 0.779 0.221 F.Crypt 0 1671 350 2.744 1.965 0.891 0.109 F.Crypt 0 3564 2640 4.917 3.851 0.739 0.261 F.Crypt 0 2196 511 3.312 3.323 0.810 0.190 F.Crypt 0 3646 1406 6.519 5.994 0.789 0.211 F.Crypt 0 3006 3294 3.700 2.735 0.641 0.359 F.Crypt 0 3604 2719 5.252 4.673 0.664 0.336 F.Crypt 0 2245 167 2.910 2.829 0.934 0.066 F.Crypt 0 2549 1084 3.174 2.069 0.835 0.165 F.Crypt 0 3454 597 5.922 4.575 0.936 0.064 F.Crypt 0 3320 521 4.843 3.536 0.940 0.060 F.Crypt 0 2033 554 2.858 3.439 0.710 0.290 F.Crypt 0 2459 506 3.042 3.445 0.786 0.214 F.Crypt 0 2088 727 2.818 4.133 0.536 0.464 F.Crypt 0 2587 1685 3.046 2.198 0.734 0.266 F.Crypt 0 2032 506 2.896 3.270 0.756 0.244 F.Crypt 0 2260 449 3.014 3.247 0.811 0.189 F.Crypt 0 2329 276 3.061 2.836 0.908 0.092 F.Crypt 0 2063 698 3.375 4.421 0.589 0.411 F.Crypt 0 1794 389 2.610 2.032 0.873 0.127 F.Crypt 0 2512 640 3.163 2.978 0.817 0.183 F.Crypt 0 2523 1293 3.135 2.224 0.786 0.214 F.Crypt 0 2286 337 3.137 1.894 0.941 0.059 F.Crypt 0 2383 721 3.249 3.040 0.793 0.207 F.Crypt 0 2258 647 2.978 3.157 0.755 0.245 F.Crypt 0 2622 560 3.322 2.862 0.866 0.134 F.Crypt 0 1947 119 4.614 3.985 0.962 0.038 F.Crypt 0 2273 250 3.298 3.244 0.904 0.096 F.Crypt 0 3290 1485 4.071 3.414 0.777 0.223 F.Crypt 0 2670 421 3.435 2.749 0.911 0.089 F.Crypt 0 2562 1770 3.036 2.263 0.712 0.288 F.Crypt 0 3087 1931 3.545 2.881 0.717 0.283 F.Crypt 0 2953 2154 4.010 3.961 0.586 0.414 F.Crypt 0 2780 656 3.501 3.499 0.809 0.191 F.Crypt 0 2554 666 3.133 3.021 0.806 0.194 F.Crypt 0 1797 361 2.604 2.770 0.816 0.184 F.Crypt 0 3091 938 4.135 2.948 0.882 0.118 F.Crypt 0 2800 943 3.632 4.166 0.672 0.328 F.Crypt 0 1879 588 2.948 3.943 0.616 0.384 F.Crypt 0 2024 517 2.767 2.396 0.835 0.165 F.Crypt 0 1997 215 3.327 2.866 0.928 0.072 F.Crypt 0 2985 366 3.792 2.967 0.935 0.065 F.Crypt 0 3299 2614 4.083 4.024 0.568 0.432 F.Crypt 0 2007 948 3.037 3.560 0.596 0.404 F.Crypt 0 3150 2348 3.853 2.738 0.744 0.256 F.Crypt 0 3498 2880 4.789 3.365 0.765 0.235 F.Crypt 0 2180 660 2.906 4.096 0.591 0.409 F.Crypt 0 2111 714 2.713 2.627 0.758 0.242 F.Crypt 0 3478 3224 5.026 4.148 0.665 0.335 F.Crypt_hiFos 0 1049 1083 4.022 3.446 0.591 0.409 F.Crypt_hiFos 0 844 278 3.112 3.507 0.698 0.302 F.Crypt_hiFos 0 1134 794 7.597 5.955 0.817 0.183 F.Crypt_hiFos 0 1134 1087 6.856 5.919 0.666 0.334 F.Crypt_hiFos 0 1105 818 4.389 3.853 0.662 0.338 F.Crypt_hiFos 0 1111 784 4.675 3.976 0.697 0.303 F.Crypt_hiFos 0 1108 687 5.225 4.744 0.692 0.308 F.Crypt_hiFos 0 795 197 5.246 4.437 0.876 0.124 F.Crypt_hiFos 0 1136 1213 6.608 5.024 0.737 0.263 F.Crypt_hiFos 0 997 782 3.471 3.886 0.489 0.511 F.Crypt_hiFos 0 1083 826 3.970 4.166 0.534 0.466 F.Crypt_hiFos 0 1080 848 4.301 4.422 0.539 0.461 F.Crypt_hiFos 0 1001 860 3.368 3.938 0.440 0.560 F.Crypt_hiFos 0 1120 2480 4.771 3.249 0.565 0.435 F.Crypt_hiFos 0 936 514 3.479 3.169 0.693 0.307 F.Crypt_hiFos 0 1136 2226 6.269 5.371 0.487 0.513 F.Crypt_hiFos 0 985 628 3.315 3.356 0.604 0.396 F.Crypt_hiFos 0 1131 817 5.879 5.050 0.711 0.289 F.Crypt_hiFos 0 1089 606 4.156 3.697 0.712 0.288 F.Crypt_hiFos 0 965 715 3.482 3.394 0.589 0.411 F.Crypt_hiFos 0 1090 2798 4.676 3.594 0.452 0.548 F.Crypt_hiFos 0 867 214 3.125 2.672 0.847 0.153 F.Crypt_hiFos 0 1126 2791 4.687 3.886 0.413 0.587 F.Crypt_hiFos 0 1141 1517 6.456 6.170 0.478 0.522 F.Crypt_hiFos 0 1126 788 6.057 5.403 0.692 0.308 F.Crypt_hiFos 0 1110 725 4.771 4.184 0.697 0.303 F.Crypt_hiFos 0 863 519 3.017 2.422 0.715 0.285 F.Crypt_hiFos 0 946 706 3.151 2.989 0.600 0.400 F.Crypt_hiFos 0 952 550 3.255 3.030 0.669 0.331 F.Crypt_hiFos 0 981 742 3.297 3.443 0.544 0.456 F.Crypt_hiFos 0 1060 1107 4.028 3.266 0.619 0.381 F.Crypt_hiFos 0 1014 526 3.617 3.403 0.691 0.309 F.Crypt_hiFos 0 1131 3028 4.716 3.536 0.458 0.542 F.Crypt_hiFos 0 1134 3268 5.166 4.234 0.398 0.602 F.Crypt_loFos_1 0 1250 1134 3.901 3.480 0.596 0.404 F.Crypt_loFos_1 0 1022 281 3.158 3.451 0.748 0.252 F.Crypt_loFos_1 0 1366 818 7.306 6.044 0.800 0.200 F.Crypt_loFos_1 0 1376 1174 7.234 5.806 0.759 0.241 F.Crypt_loFos_1 0 1327 881 4.308 3.896 0.667 0.333 F.Crypt_loFos_1 0 1332 858 4.445 4.073 0.668 0.332 F.Crypt_loFos_1 0 1216 918 3.499 3.798 0.518 0.482 F.Crypt_loFos_1 0 787 185 5.923 5.332 0.865 0.135 F.Crypt_loFos_1 0 1183 727 4.634 4.814 0.590 0.410 F.Crypt_loFos_1 0 916 204 4.830 4.778 0.823 0.177 F.Crypt_loFos_1 0 1358 1240 6.713 5.016 0.780 0.220 F.Crypt_loFos_1 0 1001 520 3.080 2.914 0.684 0.316 F.Crypt_loFos_1 0 1009 676 2.746 2.685 0.609 0.391 F.Crypt_loFos_1 0 1199 837 3.662 3.906 0.547 0.453 F.Crypt_loFos_1 0 1317 883 4.130 4.085 0.606 0.394 F.Crypt_loFos_1 0 1307 902 4.577 4.438 0.615 0.385 F.Crypt_loFos_1 0 1211 903 3.424 3.976 0.478 0.522 F.Crypt_loFos_1 0 1343 2404 4.706 3.355 0.588 0.412 F.Crypt_loFos_1 0 1090 562 3.120 3.084 0.665 0.335 F.Crypt_loFos_1 0 1023 543 3.627 3.278 0.706 0.294 F.Crypt_loFos_1 0 1364 2359 6.358 5.403 0.528 0.472 F.Crypt_loFos_1 0 1197 671 3.404 3.343 0.651 0.349 F.Crypt_loFos_1 0 1371 874 5.894 5.057 0.737 0.263 F.Crypt_loFos_1 0 898 359 2.565 2.894 0.666 0.334 F.Crypt_loFos_1 0 1301 618 4.125 3.797 0.725 0.275 F.Crypt_loFos_1 0 853 286 2.556 2.363 0.773 0.227 F.Crypt_loFos_1 0 1182 796 3.740 3.357 0.659 0.341 F.Crypt_loFos_1 0 1310 2894 4.812 3.611 0.510 0.490 F.Crypt_loFos_1 0 1370 2857 4.959 3.939 0.493 0.507 F.Crypt_loFos_1 0 1374 1612 6.526 6.130 0.529 0.471 F.Crypt_loFos_1 0 1365 2794 5.146 4.733 0.394 0.606 F.Crypt_loFos_1 0 960 350 2.743 2.988 0.698 0.302 F.Crypt_loFos_1 0 1365 826 5.956 5.358 0.714 0.286 F.Crypt_loFos_1 0 1323 795 4.867 4.057 0.745 0.255 F.Crypt_loFos_1 0 1044 692 2.856 3.290 0.528 0.472 F.Crypt_loFos_1 0 958 475 2.702 2.874 0.642 0.358 F.Crypt_loFos_1 0 1069 779 3.034 3.129 0.562 0.438 F.Crypt_loFos_1 0 1015 529 3.017 2.494 0.734 0.266 F.Crypt_loFos_1 0 1182 710 3.305 2.950 0.680 0.320 F.Crypt_loFos_1 0 996 438 3.197 3.275 0.683 0.317 F.Crypt_loFos_1 0 1300 1739 3.944 3.565 0.493 0.507 F.Crypt_loFos_1 0 1136 595 3.285 3.027 0.695 0.305 F.Crypt_loFos_1 0 1156 851 3.365 3.538 0.546 0.454 F.Crypt_loFos_1 0 1088 846 3.023 3.037 0.560 0.440 F.Crypt_loFos_1 0 1227 1199 4.022 3.296 0.629 0.371 F.Crypt_loFos_1 0 1208 1128 3.689 4.066 0.452 0.548 F.Crypt_loFos_1 0 1223 588 3.747 3.373 0.729 0.271 F.Crypt_loFos_1 0 1325 2772 4.035 4.051 0.321 0.679 F.Crypt_loFos_1 0 1294 2583 3.807 2.807 0.500 0.500 F.Crypt_loFos_1 0 1365 3132 4.845 3.565 0.514 0.486 F.Crypt_loFos_1 0 1368 3268 4.997 4.262 0.411 0.589 F.Crypt_loFos_2 0 949 1084 7.101 5.953 0.660 0.340 F.Crypt_loFos_2 0 916 1243 6.828 5.015 0.721 0.279 F.Endothelial 0 1219 273 2.908 0.994 0.944 0.056 F.Endothelial 0 1559 618 3.985 3.482 0.781 0.219 F.Endothelial 0 1441 1881 3.510 2.125 0.667 0.333 F.Endothelial 0 1556 1426 5.383 1.472 0.943 0.057 F.Endothelial 0 951 148 4.156 1.856 0.969 0.031 F.Endothelial 0 1604 2782 4.064 2.214 0.675 0.325 F.Endothelial 0 1414 49 5.228 1.567 0.997 0.003 F.Endothelial 0 1281 59 3.399 2.168 0.981 0.019 F.Endothelial 0 1643 444 4.115 2.641 0.911 0.089 F.Endothelial 0 1351 58 3.331 1.770 0.986 0.014 F.Endothelial 0 1245 368 3.311 1.973 0.895 0.105 F.Endothelial 0 1282 78 3.259 0.870 0.989 0.011 F.Endothelial 0 1635 2518 6.400 3.120 0.863 0.137 F.Endothelial 0 1644 3414 4.059 2.462 0.593 0.407 F.Endothelial 0 1334 849 3.624 3.301 0.663 0.337 F.Endothelial 0 1722 601 4.684 2.860 0.910 0.090 F.Endothelial 0 1928 6769 5.707 4.574 0.384 0.616 F.Endothelial 0 1718 4543 4.333 3.002 0.488 0.512 F.Endothelial 0 1893 2711 5.196 3.748 0.656 0.344 F.Endothelial 0 1500 1206 3.811 1.626 0.850 0.150 F.Endothelial 0 1914 1455 6.984 5.874 0.739 0.261 F.Endothelial 0 1805 5038 5.020 3.334 0.536 0.464 F.Endothelial 0 1054 47 3.046 1.581 0.984 0.016 F.Endothelial 0 1345 206 4.033 2.843 0.937 0.063 F.Endothelial 0 1289 996 3.201 1.726 0.782 0.218 F.Endothelial 0 1579 72 5.687 1.269 0.998 0.002 F.Endothelial 0 1528 143 4.279 1.597 0.986 0.014 F.Endothelial 0 1331 15 3.868 0.963 0.998 0.002 F.Endothelial 0 1006 128 3.109 2.540 0.921 0.079 F.Endothelial 0 1676 3525 4.151 2.590 0.584 0.416 F.Endothelial 0 1305 906 4.166 1.802 0.881 0.119 F.Endothelial 0 1602 512 4.493 3.167 0.887 0.113 F.Endothelial 0 1513 909 4.155 3.150 0.770 0.230 F.Endothelial 0 905 47 3.234 1.512 0.985 0.015 F.Endothelial 0 1244 15 3.544 1.783 0.996 0.004 F.Endothelial_1 0 652 1575 5.796 2.413 0.812 0.188 F.Endothelial_1 0 585 172 5.192 4.948 0.801 0.199 F.Endothelial_1 0 654 2665 6.229 3.695 0.587 0.413 F.Endothelial_1 0 676 750 4.828 3.440 0.702 0.298 F.Endothelial_1 0 586 1320 4.051 2.045 0.641 0.359 F.Endothelial_1 0 666 217 5.705 5.102 0.823 0.177 F.Fibroblast 0 4029 635 3.832 3.104 0.913 0.087 F.Fibroblast 0 3456 408 6.974 2.269 0.995 0.005 F.Fibroblast 0 4106 607 6.605 4.675 0.963 0.037 F.Fibroblast 0 3267 73 3.344 1.646 0.993 0.007 F.Fibroblast 0 4326 213 4.183 2.021 0.989 0.011 F.Fibroblast 0 4410 163 4.300 2.446 0.990 0.010 F.Fibroblast 0 4239 261 3.842 3.442 0.955 0.045 F.Fibroblast 0 1873 92 5.972 1.932 0.997 0.003 F.Fibroblast 0 1422 59 5.806 1.785 0.997 0.003 F.Fibroblast 0 2929 351 4.833 4.585 0.908 0.092 F.Fibroblast 0 1563 61 4.966 2.517 0.993 0.007 F.Fibroblast 0 5111 5338 5.197 4.037 0.681 0.319 F.Fibroblast 0 3949 704 6.211 2.064 0.990 0.010 F.Fibroblast 0 2740 114 3.128 2.120 0.980 0.020 F.Fibroblast 0 2962 197 2.886 1.903 0.967 0.033 F.Fibroblast 0 4125 199 3.894 2.397 0.983 0.017 F.Fibroblast 0 4518 186 4.169 2.996 0.982 0.018 F.Fibroblast 0 4579 172 4.539 2.685 0.990 0.010 F.Fibroblast 0 3657 165 3.437 2.078 0.983 0.017 F.Fibroblast 0 4478 190 4.006 2.265 0.987 0.013 F.Fibroblast 0 3827 2143 4.427 2.818 0.845 0.155 F.Fibroblast 0 2679 184 3.600 2.643 0.966 0.034 F.Fibroblast 0 5077 1724 6.700 2.109 0.986 0.014 F.Fibroblast 0 3686 97 3.433 2.581 0.986 0.014 F.Fibroblast 0 4311 182 5.480 1.697 0.997 0.003 F.Fibroblast 0 2121 249 3.980 1.133 0.984 0.016 F.Fibroblast 0 3905 2725 3.376 2.406 0.737 0.263 F.Fibroblast 0 2953 59 2.846 1.676 0.991 0.009 F.Fibroblast 0 3645 58 3.945 1.554 0.997 0.003 F.Fibroblast 0 2584 465 2.863 4.368 0.662 0.338 F.Fibroblast 0 3550 254 3.635 2.703 0.964 0.036 F.Fibroblast 0 4136 2346 4.358 3.393 0.775 0.225 F.Fibroblast 0 4971 2195 4.744 3.624 0.831 0.169 F.Fibroblast 0 3046 212 3.466 2.742 0.960 0.040 F.Fibroblast 0 5121 933 6.266 6.102 0.860 0.140 F.Fibroblast 0 2401 139 2.800 2.555 0.953 0.047 F.Fibroblast 0 4228 3014 3.706 2.526 0.761 0.239 F.Fibroblast 0 5158 2426 5.537 4.140 0.848 0.152 F.Fibroblast 0 3920 2336 3.479 2.320 0.789 0.211 F.Fibroblast 0 3415 811 3.148 1.349 0.936 0.064 F.Fibroblast 0 4072 234 5.743 1.786 0.996 0.004 F.Fibroblast 0 4268 103 4.481 1.355 0.997 0.003 F.Fibroblast 0 2988 230 3.363 2.578 0.957 0.043 F.Fibroblast 0 3714 77 3.343 1.563 0.994 0.006 F.Fibroblast 0 3349 331 3.886 3.831 0.913 0.087 F.Fibroblast 0 3281 1352 3.054 1.920 0.842 0.158 F.Fibroblast 0 2747 228 3.114 2.952 0.931 0.069 F.Fibroblast 0 2564 75 2.996 2.370 0.981 0.019 F.Fibroblast 0 3283 345 4.326 3.405 0.947 0.053 F.Fibroblast 0 2891 416 3.084 3.061 0.876 0.124 F.Fibroblast 0 3402 334 3.328 2.179 0.958 0.042 F.Fibroblast 0 2975 375 3.145 3.035 0.895 0.105 F.Fibroblast 0 3329 204 3.271 2.174 0.972 0.028 F.Fibroblast 0 2585 54 3.301 2.573 0.988 0.012 F.Fibroblast 0 4613 988 4.226 2.277 0.947 0.053 F.Fibroblast 0 3032 169 3.280 2.058 0.977 0.023 F.Fibroblast 0 3516 1433 3.177 1.918 0.855 0.145 F.Fibroblast 0 2875 151 3.076 2.437 0.967 0.033 F.Fibroblast 0 4317 1602 3.686 2.347 0.872 0.128 F.Fibroblast 0 3857 273 3.650 2.531 0.968 0.032 F.Fibroblast 0 3417 364 3.186 2.451 0.940 0.060 F.Fibroblast 0 3733 634 4.046 2.123 0.957 0.043 F.Fibroblast 0 4160 540 3.881 4.055 0.872 0.128 F.Fibroblast 0 3510 61 3.541 2.220 0.993 0.007 F.Fibroblast 0 4636 2280 4.656 3.474 0.822 0.178 F.Fibroblast 0 2901 671 3.427 3.580 0.795 0.205 F.Fibroblast 0 4235 1927 3.787 2.310 0.859 0.141 F.Fibroblast 0 4918 2415 4.735 2.770 0.888 0.112 F.Fibroblast 0 3694 196 3.854 3.302 0.965 0.035 F.Fibroblast 0 2773 496 2.761 2.469 0.873 0.127 F.Fibroblast 0 4853 3142 4.876 3.992 0.740 0.260 F.Glia 0 348 875 5.078 1.800 0.794 0.206 F.Glia 0 412 3823 5.854 3.599 0.340 0.660 F.Glia 0 380 452 5.884 3.738 0.788 0.212 F.Glia 0 422 256 6.580 2.417 0.967 0.033 F.Glia 0 377 118 5.034 3.083 0.925 0.075 F.Microvascular 0 395 1567 5.613 2.622 0.667 0.333 F.Microvascular 0 403 2618 7.296 3.566 0.671 0.329 F.Microvascular 0 405 241 6.509 4.671 0.857 0.143 F.Myofibroblasts 0 594 552 6.751 3.937 0.883 0.117 F.Myofibroblasts 0 586 486 6.561 3.942 0.881 0.119 F.Stromal 0 4699 323 3.769 2.021 0.980 0.020 F.Stromal 0 3224 434 6.862 2.089 0.995 0.005 F.Stromal 0 3873 667 6.467 4.709 0.952 0.048 F.Stromal 0 2981 52 3.325 1.280 0.996 0.004 F.Stromal 0 4083 1908 3.402 2.549 0.794 0.206 F.Stromal 0 4219 125 4.112 1.466 0.995 0.005 F.Stromal 0 4206 92 4.244 1.369 0.997 0.003 F.Stromal 0 4456 52 3.803 1.491 0.998 0.002 F.Stromal 0 3138 223 4.997 3.309 0.978 0.022 F.Stromal 0 1341 40 4.975 2.629 0.994 0.006 F.Stromal 0 6062 5255 5.051 3.987 0.707 0.293 F.Stromal 0 3536 750 6.157 1.994 0.988 0.012 F.Stromal 0 2758 202 2.865 1.552 0.971 0.029 F.Stromal 0 3999 99 3.904 0.760 0.997 0.003 F.Stromal 0 4386 98 4.164 1.264 0.997 0.003 F.Stromal 0 4396 114 4.521 1.678 0.996 0.004 F.Stromal 0 3587 69 3.430 1.068 0.996 0.004 F.Stromal 0 4371 87 3.975 1.532 0.996 0.004 F.Stromal 0 3962 2146 4.285 2.821 0.836 0.164 F.Stromal 0 2689 96 3.499 1.539 0.991 0.009 F.Stromal 0 5009 1743 6.560 2.060 0.985 0.015 F.Stromal 0 3480 42 3.414 1.739 0.996 0.004 F.Stromal 0 3982 197 5.413 1.504 0.997 0.003 F.Stromal 0 4636 2608 3.343 2.255 0.791 0.209 F.Stromal 0 3294 56 3.917 1.115 0.998 0.002 F.Stromal 0 3587 86 3.720 1.424 0.995 0.005 F.Stromal 0 3544 121 3.603 0.980 0.994 0.006 F.Stromal 0 4983 2076 4.421 2.935 0.871 0.129 F.Stromal 0 5515 3101 4.283 2.766 0.836 0.164 F.Stromal 0 3508 1426 3.269 2.276 0.830 0.170 F.Stromal 0 6010 1863 4.863 2.442 0.945 0.055 F.Stromal 0 3172 92 3.461 1.376 0.993 0.007 F.Stromal 0 6201 540 6.457 1.796 0.997 0.003 F.Stromal 0 4943 2914 3.611 2.444 0.792 0.208 F.Stromal 0 5847 2307 5.474 3.855 0.886 0.114 F.Stromal 0 3341 737 3.113 1.004 0.951 0.049 F.Stromal 0 3754 257 5.716 1.713 0.996 0.004 F.Stromal 0 3881 115 4.406 1.112 0.997 0.003 F.Stromal 0 3445 45 3.320 1.498 0.996 0.004 F.Stromal 0 3697 112 3.933 1.190 0.995 0.005 F.Stromal 0 3599 159 4.283 2.060 0.991 0.009 F.Stromal 0 3125 275 3.367 1.958 0.968 0.032 F.Stromal 0 3323 277 3.311 1.743 0.973 0.027 F.Stromal 0 3562 99 3.208 1.151 0.993 0.007 F.Stromal 0 3247 133 3.161 2.329 0.978 0.022 F.Stromal 0 4497 900 4.201 1.891 0.961 0.039 F.Stromal 0 2947 118 3.219 1.504 0.988 0.012 F.Stromal 0 4640 1511 3.613 2.214 0.890 0.110 F.Stromal 0 3498 279 3.641 2.437 0.967 0.033 F.Stromal 0 3728 181 3.137 1.846 0.981 0.019 F.Stromal 0 3590 561 4.073 1.321 0.977 0.023 F.Stromal 0 5071 127 4.105 1.102 0.997 0.003 F.Stromal 0 3314 63 3.793 1.337 0.997 0.003 F.Stromal 0 3169 39 3.500 0.992 0.998 0.002 F.Stromal 0 5320 2150 4.570 3.528 0.836 0.164 F.Stromal 0 3633 337 3.716 2.230 0.968 0.032 F.Stromal 0 4059 1930 3.743 2.244 0.856 0.144 F.Stromal 0 4772 2353 4.676 2.747 0.885 0.115 F.Stromal 0 3627 105 3.869 1.411 0.995 0.005 F.Stromal 0 3246 314 2.721 2.032 0.943 0.057 F.Stromal 0 5801 3009 4.853 3.850 0.794 0.206 F.Villus 0 1118 113 3.482 3.031 0.931 0.069 F.Villus 0 1755 429 3.858 2.664 0.903 0.097 F.Villus 0 1620 749 3.772 4.170 0.621 0.379 F.Villus 0 1785 760 3.998 3.616 0.754 0.246 F.Villus 0 1634 619 3.845 3.580 0.760 0.240 F.Villus 0 1701 774 3.820 4.191 0.630 0.370 F.Villus 0 1799 792 4.333 4.445 0.678 0.322 F.Villus 0 1785 592 3.789 3.151 0.824 0.176 F.Villus 0 1952 738 4.298 3.740 0.796 0.204 F.Villus 0 2185 2158 7.330 4.679 0.864 0.136 F.Villus 0 1641 565 3.540 3.345 0.769 0.231 F.Villus 0 1599 390 4.467 2.254 0.950 0.050 F.Villus 0 1319 208 3.234 2.430 0.917 0.083 F.Villus 0 1354 66 3.310 2.408 0.975 0.025 F.Villus 0 1575 269 3.591 1.921 0.949 0.051 F.Villus 0 1792 403 4.335 2.595 0.937 0.063 F.Villus 0 1669 662 3.683 3.272 0.770 0.230 F.Villus 0 1624 1098 3.742 2.252 0.806 0.194 F.Villus 0 2046 2669 4.561 3.963 0.537 0.463 F.Villus 0 1420 317 4.194 3.145 0.903 0.097 F.Villus 0 2089 1461 5.894 6.223 0.532 0.468 F.Villus 0 2165 2685 5.737 4.614 0.637 0.363 F.Villus 0 1608 676 3.810 4.416 0.610 0.390 F.Villus 0 1738 548 3.702 3.101 0.828 0.172 F.Villus 0 1617 2123 3.864 2.021 0.732 0.268 F.Villus 0 1545 159 3.557 2.182 0.962 0.038 F.Villus 0 1979 606 5.011 3.416 0.908 0.092 F.Villus 0 1771 333 4.989 3.348 0.943 0.057 F.Villus 0 1988 1564 4.363 3.326 0.723 0.277 F.Villus 0 1508 496 3.401 2.790 0.823 0.177 F.Villus 0 1642 703 3.859 3.280 0.777 0.223 F.Villus 0 1738 991 3.973 4.056 0.624 0.376 F.Villus 0 1939 2612 4.926 3.772 0.623 0.377 F.Villus 0 2050 2924 4.861 3.433 0.654 0.346 F.Villus 0 1657 632 3.869 3.723 0.744 0.256 F.Villus 0 1203 24 3.408 2.581 0.989 0.011 F.Villus_1 0 982 2294 7.382 5.226 0.656 0.344 F.Villus_1 0 836 564 4.269 3.244 0.751 0.249 F.Villus_1 0 886 791 4.923 3.822 0.706 0.294 F.Villus_1 0 858 467 5.104 3.865 0.813 0.187 F.Villus_2 0 969 549 3.899 2.999 0.767 0.233 F.Villus_2 0 1084 884 4.389 3.824 0.645 0.355 F.Villus_2 0 1203 2333 7.286 5.180 0.690 0.310 F.Villus_2 0 884 511 4.521 3.079 0.825 0.175 F.Villus_2 0 864 374 3.665 2.638 0.825 0.175 F.Villus_2 0 956 509 4.390 3.149 0.816 0.184 F.Villus_2 0 947 645 3.695 3.037 0.698 0.302 F.Villus_2 0 813 275 3.551 2.916 0.821 0.179 F.Villus_2 0 1093 757 5.078 3.833 0.774 0.226 F.Villus_2 0 1105 1727 4.490 3.435 0.571 0.429 I.Immune 0 6020 912 4.060 2.685 0.945 0.055 I.Immune 0 2923 198 5.993 1.342 0.997 0.003 I.Immune 0 3578 85 3.206 1.336 0.994 0.006 I.Immune 0 3612 91 4.454 1.223 0.997 0.003 I.Immune 0 3063 50 3.608 1.035 0.997 0.003 I.Immune 0 5000 160 4.518 1.339 0.996 0.004 I.Immune 0 3952 245 4.383 1.564 0.991 0.009 I.Immune 0 2831 115 4.230 1.067 0.995 0.005 I.Immune 0 4900 234 3.876 1.264 0.992 0.008 I.Immune 0 1786 6623 5.707 4.195 0.435 0.565 I.Immune 0 6213 4853 4.296 3.229 0.728 0.272 I.Immune 0 3302 276 3.332 1.746 0.973 0.027 I.Immune 0 3552 79 3.464 0.713 0.997 0.003 I.Immune 0 3745 128 3.391 1.254 0.992 0.008 I.Immune 0 3265 181 4.581 1.703 0.993 0.007 I.Immune 0 4538 170 3.795 0.812 0.995 0.005 I.Immune 0 3824 294 3.168 0.746 0.986 0.014 I.Immune 0 4472 331 4.275 2.045 0.984 0.016 I.Immune 0 5777 805 4.342 3.298 0.937 0.063 I.Immune 0 3800 145 4.546 1.690 0.995 0.005 I.Lymphoid 0 6125 1705 4.081 3.443 0.848 0.152 I.Lymphoid 0 3441 211 5.946 1.275 0.998 0.002 I.Lymphoid 0 3474 55 3.773 1.342 0.997 0.003 I.Lymphoid 0 4459 84 4.452 1.570 0.997 0.003 I.Lymphoid 0 3794 36 3.590 1.424 0.998 0.002 I.Lymphoid 0 5543 633 4.577 3.224 0.957 0.043 I.Lymphoid 0 4340 623 4.262 4.865 0.821 0.179 I.Lymphoid 0 3425 123 4.186 1.085 0.996 0.004 I.Lymphoid 0 5360 766 3.943 2.738 0.942 0.058 I.Lymphoid 0 3266 302 2.824 1.917 0.953 0.047 I.Lymphoid 0 3701 469 3.393 1.843 0.959 0.041 I.Lymphoid 0 5118 2541 5.374 3.490 0.881 0.119 I.Lymphoid 0 3944 330 4.659 3.021 0.974 0.026 I.Lymphoid 0 5618 178 3.758 1.359 0.994 0.006 I.Lymphoid 0 4248 586 3.189 2.168 0.936 0.064 I.Lymphoid 0 4692 364 4.507 2.525 0.981 0.019 I.Lymphoid 0 4741 147 4.535 1.971 0.995 0.005 M.CD69pos Mast 0 1123 6490 6.312 4.300 0.411 0.589 M.CD69pos Mast 0 993 3547 5.806 3.295 0.615 0.385 M.CD69pos Mast 0 813 2506 4.718 2.379 0.621 0.379 M.CD69pos Mast 0 1124 144 9.027 7.355 0.961 0.039 M.CD69pos Mast 0 835 630 4.462 1.515 0.911 0.089 M.DCs 0 751 463 4.164 4.386 0.582 0.418 M.DCs 0 794 3651 8.113 5.410 0.586 0.414 M.DCs 0 690 242 3.712 2.844 0.839 0.161 M.DCs 0 792 4441 7.237 4.407 0.559 0.441 M.DCs 0 759 1369 3.847 2.861 0.523 0.477 M.DCs 0 705 637 3.162 3.124 0.532 0.468 M.DCs 0 793 1729 6.636 4.414 0.681 0.319 M.DCs 0 792 1535 6.940 4.638 0.718 0.282 M.DCs 0 785 775 5.480 4.250 0.704 0.296 M.DCs 0 781 1025 4.857 3.358 0.683 0.317 M.DCs 0 794 1950 7.880 5.598 0.665 0.335 M.DCs 0 794 2305 6.995 4.605 0.644 0.356 M.DCs 0 727 1079 5.291 3.724 0.666 0.334 M.DCs 0 713 452 3.452 3.275 0.641 0.359 M.DCs 0 761 779 6.025 4.610 0.723 0.277 M.Macrophages 0 1259 981 4.367 2.516 0.822 0.178 M.Macrophages 0 1604 315 4.880 3.984 0.905 0.095 M.Macrophages 0 1604 193 6.399 4.403 0.971 0.029 M.Macrophages 0 1551 182 6.180 4.112 0.973 0.027 M.Macrophages 0 1591 168 5.922 4.068 0.972 0.028 M.Macrophages 0 1779 3605 7.519 5.211 0.710 0.290 M.Macrophages 0 1706 4504 6.494 4.310 0.632 0.368 M.Macrophages 0 1350 2231 4.318 2.083 0.740 0.260 M.Macrophages 0 1380 2970 4.750 2.506 0.688 0.312 M.Macrophages 0 1138 1656 3.421 1.644 0.702 0.298 M.Macrophages 0 1616 5507 5.357 3.728 0.476 0.524 M.Macrophages 0 1356 167 4.750 3.405 0.954 0.046 M.Macrophages 0 1529 569 4.931 4.204 0.816 0.184 M.Macrophages 0 1354 3286 4.180 2.604 0.551 0.449 M.Macrophages 0 1792 7034 9.465 5.572 0.791 0.209 M.Macrophages 0 1114 1352 4.300 1.573 0.845 0.155 M.Macrophages 0 1628 3460 4.771 2.665 0.669 0.331 M.Macrophages 0 1398 1302 4.047 2.615 0.743 0.257 M.Macrophages 0 1249 553 3.713 2.569 0.833 0.167 M.Macrophages 0 1696 1686 6.184 4.077 0.813 0.187 M.Macrophages 0 1741 1435 6.354 4.449 0.820 0.180 M.Macrophages 0 1587 646 5.108 3.988 0.842 0.158 M.Macrophages 0 1440 922 4.304 3.316 0.756 0.244 M.Macrophages 0 1770 1877 7.374 5.256 0.804 0.196 M.Macrophages 0 1741 2216 6.563 4.333 0.787 0.213 M.Macrophages 0 1331 1031 5.158 3.414 0.812 0.188 M.Macrophages 0 1000 96 3.324 2.648 0.943 0.057 M.Macrophages 0 1129 1343 3.886 1.713 0.791 0.209 M.Macrophages 0 1271 364 3.376 3.304 0.786 0.214 M.Macrophages 0 1511 670 5.912 4.114 0.887 0.113 M.Macrophages 0 890 68 2.914 1.915 0.963 0.037 M.Macrophages 0 1342 175 4.006 3.216 0.930 0.070 M.Macrophages 0 1099 121 3.368 2.594 0.940 0.060 M.Macrophages 0 1572 3624 4.921 2.750 0.661 0.339 M.Macrophages 0 1546 3595 5.063 2.492 0.719 0.281 M.Macrophages 0 1008 1558 5.248 2.858 0.772 0.228 M.Macrophages 0 1245 2803 3.727 2.193 0.563 0.437 M.Macrophages 0 1527 4245 4.435 3.320 0.438 0.562 M.Macrophages 0 1671 4532 5.541 3.360 0.626 0.374 M.Macrophages 0 1471 2221 5.315 3.691 0.671 0.329 M.Macrophages 0 898 90 2.765 1.742 0.953 0.047 M.Macrophages 0 1801 7464 8.586 7.077 0.407 0.593 M.Macrophages 0 1631 568 5.310 4.061 0.872 0.128 M.Mast 0 892 2099 4.344 2.247 0.645 0.355 M.Mast 0 1265 6569 6.234 4.296 0.425 0.575 M.Mast 0 1076 3546 5.738 3.286 0.624 0.376 M.Mast 0 869 2424 4.659 2.349 0.640 0.360 M.Mast 0 1269 116 9.035 3.446 0.998 0.002 M.Mast 0 965 593 4.446 0.972 0.948 0.052 M.Monocytes 0 1897 874 4.019 2.490 0.862 0.138 M.Monocytes 0 2857 156 4.719 2.195 0.991 0.009 M.Monocytes 0 1815 508 2.944 3.082 0.764 0.236 M.Monocytes 0 2307 114 6.165 2.078 0.997 0.003 M.Monocytes 0 2133 103 5.989 2.142 0.997 0.003 M.Monocytes 0 2209 95 5.739 2.159 0.996 0.004 M.Monocytes 0 1463 275 2.488 2.625 0.829 0.171 M.Monocytes 0 3091 3493 7.652 4.889 0.857 0.143 M.Monocytes 0 2424 2140 3.732 2.793 0.685 0.315 M.Monocytes 0 1908 80 3.354 1.253 0.990 0.010 M.Monocytes 0 3008 4313 6.722 4.040 0.817 0.183 M.Monocytes 0 2157 2153 3.992 1.897 0.811 0.189 M.Monocytes 0 2909 5455 5.153 3.680 0.597 0.403 M.Monocytes 0 2106 64 4.561 1.775 0.996 0.004 M.Monocytes 0 1712 141 2.960 2.399 0.947 0.053 M.Monocytes 0 2662 401 4.673 4.038 0.912 0.088 M.Monocytes 0 1818 292 2.889 2.044 0.918 0.082 M.Monocytes 0 3110 7054 9.015 5.357 0.848 0.152 M.Monocytes 0 2856 3292 4.577 2.548 0.780 0.220 M.Monocytes 0 2563 1179 3.945 2.455 0.859 0.141 M.Monocytes 0 2288 465 3.482 2.480 0.908 0.092 M.Monocytes 0 2982 1495 6.259 3.531 0.930 0.070 M.Monocytes 0 3026 1289 6.486 3.739 0.940 0.060 M.Monocytes 0 2772 544 5.172 3.422 0.945 0.055 M.Monocytes 0 1395 205 3.329 2.362 0.930 0.070 M.Monocytes 0 2620 767 4.448 2.817 0.914 0.086 M.Monocytes 0 1336 110 2.684 2.345 0.939 0.061 M.Monocytes 0 3082 1688 7.493 4.610 0.931 0.069 M.Monocytes 0 3046 2056 6.647 3.831 0.913 0.087 M.Monocytes 0 2468 850 5.151 2.923 0.932 0.068 M.Monocytes 0 1602 70 4.341 1.876 0.992 0.008 M.Monocytes 0 1725 547 2.594 2.639 0.754 0.246 M.Monocytes 0 2208 1427 3.181 3.343 0.580 0.420 M.Monocytes 0 2760 2651 5.009 4.777 0.550 0.450 M.Monocytes 0 2437 224 3.487 2.716 0.949 0.051 M.Monocytes 0 2709 513 5.972 2.582 0.982 0.018 M.Monocytes 0 2287 51 3.900 2.227 0.993 0.007 M.Monocytes 0 1745 54 3.150 2.092 0.985 0.015 M.Monocytes 0 2775 3440 4.601 2.716 0.749 0.251 M.Monocytes 0 1744 855 3.547 2.139 0.844 0.156 M.Monocytes 0 2672 3468 4.656 2.351 0.792 0.208 M.Monocytes 0 2279 1706 3.213 2.735 0.651 0.349 M.Monocytes 0 1651 203 2.735 1.357 0.955 0.045 M.Monocytes 0 2301 2679 3.514 2.173 0.685 0.315 M.Monocytes 0 2739 4164 4.264 3.231 0.574 0.426 M.Monocytes 0 2962 4464 5.344 3.186 0.748 0.252 M.Monocytes 0 2057 196 2.895 1.824 0.957 0.043 M.Monocytes 0 3122 7474 8.491 7.064 0.529 0.471 M.Monocytes 0 2380 2020 3.528 2.135 0.756 0.244 M.Monocytes 0 2822 362 5.067 3.625 0.955 0.045 M.Myeloid 0 2919 140 4.702 2.218 0.992 0.008 M.Myeloid 0 2321 124 6.159 1.666 0.998 0.002 M.Myeloid 0 2150 125 5.980 1.824 0.997 0.003 M.Myeloid 0 2223 93 5.732 1.822 0.997 0.003 M.Myeloid 0 3288 3628 7.571 4.821 0.859 0.141 M.Myeloid 0 3580 4368 6.509 4.044 0.819 0.181 M.Myeloid 0 3625 5451 4.985 3.677 0.622 0.378 M.Myeloid 0 2111 81 4.559 1.796 0.994 0.006 M.Myeloid 0 3593 235 4.604 3.771 0.965 0.035 M.Myeloid 0 4393 7356 7.972 6.710 0.589 0.411 M.Myeloid 0 4387 7036 8.638 5.278 0.865 0.135 M.Myeloid 0 2545 1392 3.591 1.731 0.869 0.131 M.Myeloid 0 3403 3404 4.467 2.435 0.804 0.196 M.Myeloid 0 2644 1244 3.926 2.383 0.861 0.139 M.Myeloid 0 2300 439 3.484 2.295 0.923 0.077 M.Myeloid 0 3135 1526 6.198 3.482 0.931 0.069 M.Myeloid 0 3111 1304 6.454 3.554 0.947 0.053 M.Myeloid 0 2798 529 5.165 3.338 0.949 0.051 M.Myeloid 0 1400 208 3.331 2.234 0.935 0.065 M.Myeloid 0 2648 787 4.439 2.881 0.908 0.092 M.Myeloid 0 3181 1708 7.454 4.571 0.932 0.068 M.Myeloid 0 3202 2024 6.585 3.810 0.915 0.085 M.Myeloid 0 2535 866 5.121 2.926 0.931 0.069 M.Myeloid 0 2494 230 3.483 3.035 0.937 0.063 M.Myeloid 0 2749 527 5.960 2.455 0.983 0.017 M.Myeloid 0 2300 48 3.900 1.788 0.995 0.005 M.Myeloid 0 3387 3537 4.481 2.615 0.777 0.223 M.Myeloid 0 3206 3517 4.532 2.297 0.811 0.189 M.Myeloid 0 3391 4180 4.220 3.215 0.620 0.380 M.Myeloid 0 3745 4510 5.191 3.125 0.777 0.223 M.Myeloid 0 3737 2618 4.753 4.074 0.696 0.304 M.Myeloid 0 4407 7468 8.202 7.029 0.571 0.429 M.Myeloid 0 3501 255 4.897 3.573 0.972 0.028 M.Tissue_DCs 0 643 481 4.281 4.460 0.541 0.459 M.Tissue_DCs 0 672 3634 8.013 5.364 0.537 0.463 M.Tissue_DCs 0 578 146 3.803 3.080 0.867 0.133 M.Tissue_DCs 0 670 4472 7.124 4.451 0.489 0.511 M.Tissue_DCs 0 643 1368 3.884 2.767 0.505 0.495 M.Tissue_DCs 0 671 1759 6.577 4.420 0.630 0.370 M.Tissue_DCs 0 670 1484 6.863 4.773 0.658 0.342 M.Tissue_DCs 0 663 738 5.457 4.290 0.669 0.331 M.Tissue_DCs 0 662 1000 4.815 3.367 0.644 0.356 M.Tissue_DCs 0 672 1937 7.874 5.574 0.631 0.369 M.Tissue_DCs 0 672 2279 6.984 4.587 0.608 0.392 M.Tissue_DCs 0 622 462 3.581 3.366 0.610 0.390 M.Tissue_DCs 0 640 782 6.080 4.547 0.703 0.297 T.CD4 0 5187 2552 4.312 3.578 0.772 0.228 T.CD4 0 6115 7425 7.908 6.955 0.615 0.385 T.CD4 0 5262 4406 4.793 3.354 0.764 0.236 T.CD4 0 4067 522 3.823 3.702 0.894 0.106 T.CD4 0 5156 643 4.361 4.376 0.888 0.112 T.CD4 0 4233 549 3.570 3.491 0.891 0.109 T.CD4 0 5137 1523 4.538 4.307 0.798 0.202 T.CD4 0 6074 7227 6.822 5.836 0.625 0.375 T.CD4 0 5533 2804 5.278 4.263 0.800 0.200 T.CD4 0 4588 886 4.766 4.230 0.883 0.117 T.CD4 0 6079 7288 7.129 6.260 0.604 0.396 T.CD4 0 5989 6942 6.135 5.158 0.629 0.371 T.CD4 0 6061 7192 6.695 5.717 0.624 0.376 T.CD4 0 6034 7017 6.324 5.430 0.615 0.385 T.CD4 0 5855 6596 5.349 4.369 0.637 0.363 T.CD4 0 6030 7028 6.381 5.184 0.663 0.337 T.CD4 0 5927 6769 5.913 4.944 0.631 0.369 T.CD4 0 5988 6999 6.052 5.244 0.600 0.400 T.CD4 0 4285 3675 3.757 2.468 0.740 0.260 T.CD4 0 6122 7459 7.932 7.047 0.602 0.398 T.CD4 0 5232 948 4.671 3.876 0.905 0.095 T.CD4 0 5075 837 4.719 4.066 0.905 0.095 T.CD8 0 4141 7129 6.459 5.447 0.540 0.460 T.CD8 0 3679 2662 4.342 3.756 0.675 0.325 T.CD8 0 4167 7446 8.044 7.029 0.531 0.469 T.CD8 0 3896 699 6.285 4.684 0.944 0.056 T.CD8 0 3622 1088 4.617 4.237 0.812 0.188 T.CD8 0 3183 896 3.706 3.503 0.804 0.196 T.CD8 0 3668 1773 4.811 4.187 0.761 0.239 T.CD8 0 3012 783 4.335 3.569 0.867 0.133 T.CD8 0 3458 1801 4.144 3.610 0.735 0.265 T.CD8 0 2775 1166 3.555 2.976 0.780 0.220 T.CD8 0 2956 344 5.852 4.682 0.951 0.049 T.CD8 0 3117 1132 3.782 3.025 0.823 0.177 T.CD8 0 2194 318 3.874 3.303 0.911 0.089 T.CD8 0 4007 3265 5.519 4.367 0.732 0.268 T.CD8 0 3166 315 4.585 4.231 0.928 0.072 T.CD8 0 3384 1619 4.095 3.450 0.766 0.234 T.CD8 0 3856 5624 4.736 3.749 0.576 0.424 T.CD8 0 4168 7463 8.386 7.040 0.587 0.413 T.CD8 0 3505 1405 4.545 4.333 0.743 0.257 T.CD8 0 3498 1277 4.549 4.496 0.740 0.260 T.CD8_IELs 0 1582 1004 6.549 5.273 0.792 0.208 T.CD8_IELs 0 1364 1360 4.702 4.376 0.557 0.443 T.CD8_IELs 0 1486 1995 4.865 4.341 0.517 0.483 T.CD8_IELs 0 1414 1003 4.790 3.630 0.759 0.241 T.CD8_IELs 0 1211 424 4.054 3.412 0.817 0.183 T.CD8_IELs 0 1552 3461 5.772 4.518 0.517 0.483 T.CD8_IELs 0 1311 593 4.406 4.614 0.657 0.343 T.CD8 LP 0 1849 931 6.222 5.372 0.782 0.218 T.CD8 LP 0 1523 544 4.793 4.225 0.806 0.194 T.Tcells 0 7176 7092 6.254 5.363 0.652 0.348 T.Tcells 0 6214 2208 4.290 3.309 0.847 0.153 T.Tcells 0 7263 7424 7.915 6.800 0.679 0.321 T.Tcells 0 6125 4331 4.691 3.042 0.816 0.184 T.Tcells 0 4168 350 5.968 3.879 0.981 0.019 T.Tcells 0 4718 126 3.815 2.607 0.989 0.011 T.Tcells 0 6220 143 4.461 1.922 0.996 0.004 T.Tcells 0 5275 90 3.603 2.457 0.992 0.008 T.Tcells 0 6205 1100 4.606 3.906 0.902 0.098 T.Tcells 0 4463 217 4.085 3.492 0.969 0.031 T.Tcells 0 3661 2127 3.412 1.851 0.835 0.165 T.Tcells 0 5641 1278 4.004 3.324 0.876 0.124 T.Tcells 0 4420 669 3.464 2.212 0.940 0.060 T.Tcells 0 2751 189 5.826 4.113 0.979 0.021 T.Tcells 0 4351 749 3.584 2.617 0.919 0.081 T.Tcells 0 2136 218 3.775 3.224 0.935 0.065 T.Tcells 0 3819 1590 3.287 1.717 0.877 0.123 T.Tcells 0 6717 2386 5.388 3.569 0.909 0.091 T.Tcells 0 3982 177 3.294 2.299 0.978 0.022 T.Tcells 0 4454 687 4.631 4.205 0.897 0.103 T.Tcells 0 5665 5265 4.016 3.130 0.665 0.335 T.Tcells 0 2809 225 4.479 4.344 0.932 0.068 T.Tcells 0 5519 1057 3.917 2.940 0.911 0.089 T.Tcells 0 4119 1178 3.375 2.293 0.881 0.119 T.Tcells 0 7206 7197 6.564 5.647 0.654 0.346 T.Tcells 0 7191 7013 6.286 5.318 0.667 0.333 T.Tcells 0 7181 7033 6.297 5.052 0.708 0.292 T.Tcells 0 7057 6748 5.806 4.867 0.667 0.333 T.Tcells 0 6212 5466 4.504 3.586 0.682 0.318 T.Tcells 0 4941 3660 3.646 2.209 0.785 0.215 T.Tcells 0 7271 7444 8.103 6.826 0.703 0.297 T.Tcells 0 6163 451 4.592 2.553 0.983 0.017 T.Tcells 0 6049 358 4.642 2.673 0.985 0.015

TABLE 13 Inflamed vs Healthy Markers ident gene coefD pvalD coefC pvalC mastfc B.Bcells AC009501.4 −0.840 3.95E−34 2.53E−01 2.55E−07 −0.741 B.Bcells ACAP1 1.066 1.15E−42 6.23E−01 2.91E−34 0.707 B.Bcells ACP5 0.764 2.94E−22 8.02E−01 9.84E−33 0.540 B.Bcells ACTG1 0.518 8.84E−07 1.33E+00  2.04E−185 1.239 B.Bcells ACTR3 0.992 1.10E−43 6.71E−01 2.51E−48 0.544 B.Bcells ALOX5AP 1.429 5.97E−60 4.36E−01 1.73E−10 1.430 B.Bcells ARHGDIB 0.800 1.93E−23 8.96E−01 1.64E−90 1.398 B.Bcells ARPC1B 0.824 2.50E−30 9.25E−01 1.70E−84 1.086 B.Bcells ARPC2 0.596 1.17E−08 9.73E−01  2.29E−138 0.656 B.Bcells ARPC5 1.043 3.72E−46 7.81E−01 3.25E−61 0.815 B.Bcells ATP5E 0.560 6.15E−08 7.70E−01  4.66E−104 0.767 B.Bcells BATF 2.091 1.33E−43 5.98E−01 8.77E−06 0.637 B.Bcells CAP1 0.816 9.89E−29 5.78E−01 6.04E−39 0.511 B.Bcells CAPZB 0.616 1.83E−16 7.46E−01 2.09E−66 0.575 B.Bcells CD37 0.709 1.90E−24 8.98E−01 7.79E−70 0.856 B.Bcells CD52 0.831 1.88E−32 1.34E+00  1.78E−101 1.800 B.Bcells CD53 0.836 1.56E−32 9.36E−01 3.51E−91 0.723 B.Bcells CFL1 0.552 6.13E−07 9.86E−01  2.82E−121 1.185 B.Bcells CORO1A 1.217 3.24E−65 1.17E+00 4.13E−96 1.971 B.Bcells COTL1 1.254 1.98E−62 6.23E−01 4.95E−23 1.044 B.Bcells DHRS9 2.923 1.56E−85 5.75E−01 3.94E−04 1.495 B.Bcells DUOXA2 4.226 3.70E−21 1.00E+00 2.568 B.Bcells EVL 1.158 1.79E−47 6.17E−01 1.75E−27 1.267 B.Bcells GAPDH 0.738 9.52E−08 1.03E+00  3.18E−140 1.167 B.Bcells GBP1 1.930 1.69E−33 6.71E−01 2.07E−07 0.656 B.Bcells GBP2 1.390 1.19E−22 9.89E−01 1.58E−21 0.920 B.Bcells GPSM3 0.679 8.63E−23 5.98E−01 4.20E−42 0.515 B.Bcells H3F3A 0.586 1.26E−06 7.04E−01 4.66E−76 0.772 B.Bcells HLA-DMA 1.086 8.58E−54 6.11E−01 1.35E−30 0.600 B.Bcells HLA-DPA1 0.602 1.74E−16 1.03E+00 7.98E−50 0.803 B.Bcells HLA-DPB1 0.797 5.81E−31 9.67E−01 2.04E−33 1.059 B.Bcells HLA-DQA1 0.880 5.41E−37 9.73E−01 5.18E−45 0.661 B.Bcells HLA-DRA 0.580 5.76E−16 1.16E+00 4.34E−34 0.783 B.Bcells HLA-DRB1 0.686 1.94E−22 1.17E+00 1.06E−48 0.905 B.Bcells HOPX 1.829 2.48E−45 5.15E−01 3.43E−05 1.804 B.Bcells IGHA1 −1.355 4.90E−48 −2.56E+00   7.40E−136 −2.004 B.Bcells IGHA2 −1.541 4.79E−99 −2.61E+00   2.21E−114 −0.952 B.Bcells IGJ −1.186 3.38E−47 −1.77E+00  8.06E−84 −0.915 B.Bcells ITGB2 1.489 9.36E−57 7.06E−01 3.79E−24 0.847 B.Bcells LAPTM5 1.327 2.70E−77 8.69E−01 3.53E−46 1.557 B.Bcells LCP1 1.729 2.92E−84 3.32E−01 5.59E−07 0.967 B.Bcells LIMD2 1.040 1.95E−50 9.12E−01 1.30E−62 0.786 B.Bcells LSP1 0.374 2.12E−07 6.18E−01 3.73E−62 0.502 B.Bcells LST1 1.447 3.82E−25 3.84E−01 3.07E−03 0.703 B.Bcells LTB 0.945 1.56E−39 5.70E−01 5.62E−14 1.258 B.Bcells MT-ND3 0.437 1.64E−09 9.87E−01 6.68E−38 0.631 B.Bcells MYL12A 0.262 1.13E−03 6.57E−01 2.57E−55 0.513 B.Bcells PKM 0.751 7.21E−24 8.45E−01 1.18E−69 0.595 B.Bcells PPIA 0.727 4.42E−17 7.26E−01 8.00E−72 0.781 B.Bcells PPP1R18 1.280 7.03E−49 7.09E−01 5.00E−35 0.682 B.Bcells PSMB9 0.578 2.60E−15 6.89E−01 6.34E−69 0.502 B.Bcells PTPRC 1.464 7.12E−70 4.40E−01 9.28E−13 1.071 B.Bcells PTPRCAP 0.753 8.87E−21 1.05E+00  1.61E−120 1.056 B.Bcells RAC2 0.712 2.69E−24 7.58E−01 4.61E−74 0.552 B.Bcells RPL17 −1.084 1.83E−41 −1.24E−01  6.59E−04 −0.663 B.Bcells RPS24 0.267 7.32E−02 7.49E−01 5.36E−76 0.556 B.Bcells SERF2 0.495 6.78E−03 5.69E−01 1.17E−67 0.752 B.Bcells SOCS1 1.066 8.64E−34 5.95E−01 2.20E−19 0.518 B.Bcells STMN1 0.845 9.34E−21 1.15E+00 2.85E−32 0.559 B.Bcells TTC39C 1.991 1.01E−20 2.00E−01 2.17E−01 0.651 B.Bcells UCP2 1.124 2.55E−55 6.00E−01 1.13E−27 0.688 B.Cycling ACTB 1.210 5.44E−02 2.80E+00 4.48E−85 3.533 B.Cycling ACTG1 1.344 2.46E−04 1.59E+00 2.71E−41 2.152 B.Cycling ACTR3 1.650 1.29E−13 8.00E−01 3.56E−12 1.051 B.Cycling ARHGDIB 1.737 1.49E−10 1.54E+00 7.59E−35 2.945 B.Cycling ARPC1B 1.372 1.64E−09 1.05E+00 5.92E−17 1.678 B.Cycling ARPC2 1.134 2.00E−03 1.47E+00 3.77E−46 1.514 B.Cycling ARPC3 1.198 2.47E−05 1.13E+00 1.48E−26 1.208 B.Cycling ARPC5 1.874 1.37E−16 7.33E−01 4.59E−09 1.374 B.Cycling CD53 1.217 3.35E−09 1.30E+00 4.46E−26 1.383 B.Cycling CORO1A 2.167 8.33E−21 1.63E+00 1.66E−31 3.301 B.Cycling GAPDH 3.021 2.42E−04 1.73E+00 1.17E−52 4.052 B.Cycling H2AFZ 0.760 5.45E−02 1.46E+00 3.54E−40 0.961 B.Cycling HLA-DPA1 1.450 1.27E−11 1.31E+00 8.25E−10 1.891 B.Cycling HLA-DRA 1.884 2.94E−17 1.66E+00 1.86E−09 2.805 B.Cycling HMGB1 2.006 3.96E−07 1.71E+00 6.45E−51 2.517 B.Cycling HMGB2 1.657 2.93E−12 1.13E+00 8.29E−17 1.265 B.Cycling HMGN1 1.706 4.25E−09 1.11E+00 1.15E−24 1.579 B.Cycling HMGN2 1.559 2.18E−07 1.80E+00 6.33E−57 1.922 B.Cycling HNRNPA1 0.889 1.13E−02 1.35E+00 2.77E−37 1.422 B.Cycling HNRNPA2B1 1.175 1.93E−05 1.28E+00 6.89E−32 1.187 B.Cycling HNRNPK 1.101 8.09E−06 1.04E+00 1.77E−23 0.841 B.Cycling LAPTM5 1.865 3.52E−20 8.75E−01 1.07E−08 2.088 B.Cycling LAT2 2.014 5.93E−19 4.85E−01 9.69E−03 0.632 B.Cycling LCP1 2.072 5.27E−22 −4.47E−02  7.54E−01 1.018 B.Cycling LDHA 1.530 1.23E−09 9.28E−01 7.24E−14 1.346 B.Cycling LDHB 1.097 7.52E−06 1.00E+00 8.69E−20 1.187 B.Cycling LIMD2 1.883 2.98E−20 7.23E−01 2.17E−07 1.574 B.Cycling MS4A1 2.125 1.51E−22 5.90E−01 5.47E−03 0.516 B.Cycling NAP1L1 1.046 4.82E−07 9.50E−01 4.50E−17 0.916 B.Cycling NCF1 0.935 2.95E−06 1.04E+00 4.82E−20 0.622 B.Cycling NPM1 0.917 8.69E−03 1.09E+00 3.34E−24 1.375 B.Cycling PKM 1.263 1.73E−07 1.33E+00 1.14E−28 1.033 B.Cycling RAC2 1.456 4.14E−12 1.06E+00 1.28E−18 1.554 B.Cycling RAN 1.151 1.12E−05 1.10E+00 1.24E−24 0.943 B.Cycling RPL39 0.407 6.43E−02 1.85E+00 1.29E−21 0.602 B.Cycling STMN1 1.816 2.22E−15 7.47E−01 1.12E−07 1.165 B.Cycling TUBA1B 1.809 5.39E−09 1.60E+00 3.95E−33 2.359 B.Cycling TUBB 1.915 1.40E−13 1.43E+00 5.06E−31 2.022 B.FO ACAP1 1.242 4.69E−20 3.91E−01 2.55E−06 0.810 B.FO ACP5 1.487 1.63E−28 3.10E−01 5.22E−03 0.949 B.FO ACTB 0.101 8.13E−01 1.25E+00 6.28E−44 0.799 B.FO ACTG1 0.573 3.21E−03 8.80E−01 3.05E−32 0.844 B.FO ALOX5AP 1.327 1.53E−20 8.10E−02 4.32E−01 1.142 B.FO ARHGDIB 1.129 5.19E−13 4.51E−01 1.28E−09 1.511 B.FO ARPC1B 0.705 1.42E−07 5.79E−01 1.76E−14 0.757 B.FO BATF 2.222 1.48E−21 3.48E−01 1.15E−01 0.878 B.FO BIRC3 1.205 3.46E−20 1.41E−01 1.32E−01 0.501 B.FO CD48 1.132 3.70E−19 3.05E−01 2.67E−05 0.952 B.FO CD52 0.743 2.15E−06 9.97E−01 5.23E−34 1.419 B.FO CD53 1.245 6.33E−21 4.51E−01 1.57E−10 1.043 B.FO CLEC2B 1.793 2.09E−21 3.04E−01 2.69E−02 1.020 B.FO CORO1A 1.454 2.43E−22 7.04E−01 3.11E−20 1.896 B.FO COTL1 1.048 4.20E−16 5.22E−01 8.07E−10 0.742 B.FO DHRS9 3.753 1.38E−33 5.78E−01 2.16E−01 2.150 B.FO EPSTI1 1.920 2.42E−19 1.41E−01 3.51E−01 0.503 B.FO EVL 1.416 2.07E−26 1.64E−01 5.08E−02 1.268 B.FO GBP1 2.259 2.65E−20 2.87E−01 1.59E−01 0.853 B.FO GBP2 2.682 1.37E−30 5.04E−01 9.17E−03 1.837 B.FO GBP4 3.236 3.95E−29 9.92E−02 7.16E−01 1.130 B.FO GMFG 1.019 7.41E−16 3.64E−01 1.86E−06 1.069 B.FO GYPC 1.437 8.07E−29 5.61E−01 1.60E−14 1.382 B.FO HCLS1 1.059 2.60E−15 4.10E−01 1.73E−07 0.531 B.FO HCST 1.403 3.21E−19 1.92E−01 8.82E−02 1.350 B.FO HLA-B 0.225 5.45E−01 7.46E−01 9.81E−24 0.553 B.FO HOPX 2.240 2.75E−28 4.97E−01 9.34E−03 2.321 B.FO IGJ −1.260 2.53E−23 1.53E−01 5.27E−01 −1.065 B.FO IRF1 1.113 3.14E−16 4.47E−01 5.43E−06 0.766 B.FO ITGB2 2.100 6.23E−40 1.20E−01 2.89E−01 1.190 B.FO LAPTM5 1.462 1.98E−27 5.88E−01 7.58E−16 1.526 B.FO LCP1 1.555 4.77E−26 2.13E−02 8.12E−01 0.755 B.FO LIMD2 1.238 6.56E−22 4.73E−01 7.16E−11 0.796 B.FO LSP1 1.126 2.19E−18 2.86E−01 7.86E−05 1.147 B.FO LY6E 1.309 5.92E−21 −4.74E−02  6.41E−01 1.071 B.FO PPP1R18 1.690 4.06E−29 1.40E−01 1.15E−01 0.801 B.FO PTPRC 1.577 1.92E−30 2.07E−01 1.66E−02 1.058 B.FO PTPRCAP 1.252 3.80E−17 7.36E−01 1.25E−22 1.585 B.FO RAC2 1.128 1.74E−18 3.32E−01 2.36E−06 0.899 B.FO RHOH 0.947 7.00E−14 4.86E−01 4.32E−10 0.558 B.FO RPS4Y1 0.994 6.52E−12 7.54E−01 2.92E−10 0.866 B.FO 6-Sep 1.453 5.58E−25 2.92E−01 1.55E−03 0.543 B.FO SOCS1 1.798 1.08E−25 −5.09E−02  6.99E−01 0.987 B.FO VAMP5 1.550 7.55E−21 2.74E−01 4.35E−02 1.038 B.GC ACTB 1.429 8.36E−02 1.66E+00 1.28E−20 2.884 B.GC CD52 2.524 1.96E−13 1.05E+00 7.19E−10 3.356 B.GC HLA-DQB1 2.254 2.57E−14 1.08E+00 6.51E−08 1.945 B.Plasma DHRS9 2.692 8.88E−27 9.71E−01 2.14E−04 1.535 B.Plasma IGHA1 −3.590 2.13E−23 −2.33E+00   3.21E−130 −3.007 B.Plasma IGHA2 −3.629 1.96E−55 −2.81E+00   4.82E−125 −1.563 B.Plasma IGJ −4.003 1.81E−27 −1.59E+00  2.78E−94 −1.620 B.Plasma MS4A1 2.416 2.90E−17 1.58E+00 2.93E−05 1.191 B.Plasma RGS2 −1.140 4.07E−23 −2.48E−01  1.12E−04 −0.544 B.Plasma RPL17 −1.494 1.00E−23 −1.48E−01  2.75E−03 −0.956 E.Absorptive AC009501.4 −2.051 2.54E−62 5.49E−01 9.89E−08 −1.515 E.Absorptive B2M −1.377 5.95E−02 7.43E−01 1.29E−21 −1.703 E.Absorptive BIRC3 1.039 2.28E−17 8.71E−01 3.54E−28 0.513 E.Absorptive C2 2.730 2.21E−32 3.39E−01 5.88E−02 0.892 E.Absorptive C4orf3 0.745 1.22E−07 7.64E−01 1.16E−38 0.515 E.Absorptive CA2 −1.604 6.80E−18 −7.71E−01  3.08E−18 −0.504 E.Absorptive CXCL1 3.150 1.07E−42 2.61E+00 2.15E−09 2.180 E.Absorptive F3 2.139 1.95E−20 7.40E−01 1.71E−03 0.721 E.Absorptive FSTL1 3.103 7.52E−19 1.01E+00 4.22E−03 1.251 E.Absorptive GBP4 2.153 7.68E−18 7.64E−01 1.26E−05 0.564 E.Absorptive GSN 0.648 5.56E−04 8.55E−01 3.38E−31 0.705 E.Absorptive HLA-B 0.505 3.69E−01 9.39E−01 8.66E−41 1.084 E.Absorptive HLA-DRB1 1.843 7.53E−44 1.27E+00 3.16E−26 2.336 E.Absorptive HLA-E 0.433 2.54E−02 6.42E−01 1.64E−28 0.564 E.Absorptive HSPB1 −1.796 1.84E−30 −4.37E−01  1.69E−07 −0.732 E.Absorptive IDO1 4.788 4.77E−33 1.00E+00 5.394 E.Absorptive IFI6 1.134 2.63E−10 1.05E+00 9.73E−13 0.541 E.Absorptive IFITM3 0.973 8.41E−13 1.35E+00 2.01E−33 1.180 E.Absorptive IL2RG 1.161 3.70E−21 8.22E−01 1.34E−40 0.995 E.Absorptive ITM2B 0.707 1.18E−03 9.07E−01 4.66E−44 0.935 E.Absorptive LAPTM4A 0.723 4.42E−06 8.38E−01 1.24E−36 0.501 E.Absorptive LGALS4 −0.690 2.11E−01 −7.02E−01  3.14E−20 −0.601 E.Absorptive LPCAT1 2.997 4.17E−24 5.03E−01 4.52E−02 0.520 E.Absorptive MMP7 4.751 1.86E−24 1.00E+00 5.394 E.Absorptive MUC12 1.647 3.32E−17 1.41E+00  2.18E−100 0.726 E.Absorptive PARP8 3.844 1.43E−27 −3.03E−01  5.12E−01 0.836 E.Absorptive PDLIM7 1.800 1.73E−18 7.62E−01 9.29E−09 0.596 E.Absorptive PFKFB3 2.431 9.07E−32 5.85E−01 1.06E−05 0.504 E.Absorptive PLA2G16 1.381 1.15E−15 5.83E−01 9.23E−07 0.585 E.Absorptive PLA2G2A 1.639 6.27E−32 1.55E+00 9.26E−36 0.508 E.Absorptive PNRC1 0.757 9.17E−09 7.40E−01 3.96E−26 0.579 E.Absorptive PSMB9 0.626 6.99E−06 8.54E−01 3.79E−46 0.607 E.Absorptive PSME2 1.164 6.57E−08 8.15E−01 1.40E−45 1.088 E.Absorptive RARRES3 1.558 3.64E−33 9.72E−01 9.80E−54 1.625 E.Absorptive REG4 2.931 1.55E−43 1.65E+00 5.19E−05 1.418 E.Absorptive RNASE1 1.637 6.05E−30 1.30E+00 1.50E−41 0.982 E.Absorptive S100A11 0.839 5.39E−09 1.67E+00 3.16E−88 1.341 E.Absorptive S100A6 1.276 3.38E−01 7.96E−01 2.13E−21 1.728 E.Absorptive S100A9 3.985 1.12E−37 1.99E+00 9.81E−03 1.209 E.Absorptive SEPPI 0.558 5.30E−05 1.09E+00 4.66E−33 0.759 E.Absorptive SLC25A6 −1.779 6.80E−19 −4.44E−01  1.48E−12 −0.644 E.Absorptive SLC6A14 5.158 8.49E−41 1.00E+00 5.394 E.Absorptive SOCS1 1.130 2.55E−12 1.33E+00 1.08E−27 0.710 E.Absorptive SOD3 1.634 7.87E−26 1.58E+00 2.74E−27 0.986 E.Absorptive TFF1 1.636 6.62E−37 1.62E+00 3.71E−43 0.619 E.Absorptive VAMP5 1.323 1.18E−22 7.36E−01 4.33E−15 0.969 E.Absorptive VNN1 4.531 1.58E−23 1.00E+00 5.394 E.Absorptive WARS 1.396 1.04E−14 9.54E−01 3.17E−13 0.538 E.Absorptive_All AC009501.4 −1.792  1.15E−163 4.81E−01 1.04E−22 −1.362 E.Absorptive_All AGR2 0.782 6.21E−23 1.04E+00 5.64E−84 0.507 E.Absorptive_All ANXA5 0.954 2.34E−18 6.57E−01 4.45E−13 0.676 E.Absorptive_All C2 2.754 1.09E−39 6.00E−01 4.15E−03 1.003 E.Absorptive_All COX4I1 −0.853 3.27E−12 −5.60E−01  1.37E−65 −0.604 E.Absorptive_All CXCL1 2.908 9.82E−81 2.04E+00 1.38E−10 1.577 E.Absorptive_All DAPP1 3.328 2.96E−30 7.70E−01 5.62E−02 0.582 E.Absorptive_All DDX5 0.523 3.14E−12 6.62E−01 6.50E−62 0.579 E.Absorptive_All FABP1 −2.045 3.38E−53 −6.57E−01  4.44E−27 −0.617 E.Absorptive_All FOS −0.936 1.18E−35 1.75E−01 1.10E−03 −0.671 E.Absorptive_All FSTL1 2.851 2.95E−25 9.20E−01 1.49E−03 0.968 E.Absorptive_All FTH1 −0.974 6.31E−03 −4.70E−01  1.01E−22 −1.551 E.Absorptive_All FTL −0.747 3.28E−07 −7.28E−01  2.29E−67 −1.280 E.Absorptive_All GLRA2 4.198 3.03E−23 1.00E+00 4.481 E.Absorptive_All H3F3B 0.244 8.30E−03 4.44E−01 1.01E−34 0.505 E.Absorptive_All HLA-DMA 1.347 1.29E−40 7.79E−01 1.67E−16 0.784 E.Absorptive_All HLA-DMB 1.612 3.18E−22 3.70E−01 2.49E−02 0.680 E.Absorptive_All HLA-DRB1 1.433 1.16E−88 1.14E+00 7.09E−40 1.590 E.Absorptive_All IDO1 3.952 7.80E−22 1.00E+00 4.481 E.Absorptive_All IFI16 2.247 8.22E−31 4.37E−01 1.58E−02 0.943 E.Absorptive_All IFITM3 0.685 2.16E−19 1.08E+00 6.15E−57 0.795 E.Absorptive_All IL2RG 1.007 9.58E−45 6.21E−01 2.87E−35 0.751 E.Absorptive_All JUN −1.110 8.43E−48 2.69E−03 9.54E−01 −0.593 E.Absorptive_All KYNU 3.935 1.46E−21 1.00E+00 4.481 E.Absorptive_All LYZ 1.481 4.03E−35 8.61E−01 9.01E−06 0.718 E.Absorptive_All MMP7 4.430 1.64E−23 1.00E+00 4.481 E.Absorptive_All MTRNR2L1 0.449 4.87E−11 1.43E+00 1.57E−43 0.538 E.Absorptive_All MYL6 −0.955 7.44E−12 −3.37E−01  8.80E−26 −0.673 E.Absorptive_All OLFM4 1.788 7.27E−98 1.05E+00 4.42E−22 0.655 E.Absorptive_All PARP8 3.785 6.51E−41 1.48E−01 7.36E−01 1.034 E.Absorptive_All PHGR1 −2.038 3.78E−17 −6.91E−01  4.99E−42 −0.784 E.Absorptive_All PLA2G2A 2.131  4.09E−182 1.55E+00 5.54E−96 0.758 E.Absorptive_All PPDPF −0.839 3.41E−14 −2.78E−01  3.96E−17 −0.508 E.Absorptive_All RARRES3 1.064 7.21E−50 6.87E−01 8.29E−39 1.037 E.Absorptive_All RBPMS 3.743 7.60E−47 7.07E−01 1.04E−01 2.445 E.Absorptive_All REG4 2.831  9.24E−112 1.58E+00 6.02E−09 1.812 E.Absorptive_All RNASE1 1.207 2.86E−52 9.10E−01 3.07E−53 0.765 E.Absorptive_All S100A11 1.169 6.07E−58 1.23E+00  6.71E−148 1.584 E.Absorptive_All S100A6 0.331 2.90E−01 8.55E−01 1.16E−96 0.820 E.Absorptive_All S100A9 4.103 5.97E−66 1.24E+00 8.10E−02 1.174 E.Absorptive_All S100P 3.310  5.39E−308 1.75E+00 2.53E−77 0.906 E.Absorptive_All SEPP1 0.543 5.00E−17 8.41E−01 1.28E−39 0.565 E.Absorptive_All SLC25A6 −1.053 1.01E−33 −3.60E−01  2.98E−24 −0.565 E.Absorptive_All SLC6A14 4.946 3.95E−49 1.00E+00 4.481 E.Absorptive_All SOCS1 1.315 1.57E−27 1.10E+00 3.29E−27 0.793 E.Absorptive_All SOD3 1.638 8.80E−50 1.15E+00 1.53E−20 0.926 E.Absorptive_All TFF1 1.851  1.10E−135 1.27E+00 1.20E−35 1.028 E.Absorptive_All TIMP1 3.502  8.11E−199 1.28E+00 1.56E−09 3.673 E.Absorptive_All TNIP3 4.300 2.15E−59 1.38E+00 3.48E−02 0.639 E.Absorptive_All TRIM22 2.732 1.06E−24 8.20E−01 1.73E−03 0.823 E.Absorptive_All VAMP5 1.000 1.29E−23 5.06E−01 6.45E−10 0.612 E.Absorptive_All VNN1 3.903 9.55E−19 1.00E+00 4.481 E.Absorptive_All XKR9 4.027 4.63E−21 1.00E+00 4.481 E.Absorptive_TA_1 COX4I1 −1.237 7.85E−14 −4.51E−01  1.06E−10 −0.813 E.Absorptive_TA_1 DUOX2 4.483 9.35E−22 1.00E+00 3.487 E.Absorptive_TA_1 DUOXA2 4.970 1.86E−32 1.00E+00 3.487 E.Absorptive_TA_1 LGALS3 −1.243 2.05E−15 −4.97E−01  1.55E−07 −0.764 E.Absorptive_TA_1 LGALS4 −1.865 1.50E−22 −6.63E−01  2.27E−13 −0.794 E.Absorptive_TA_1 MTRNR2L1 1.007 2.80E−13 1.46E+00 2.30E−12 1.006 E.Absorptive_TA_1 MUC12 1.924 1.08E−41 9.71E−01 2.25E−14 0.746 E.Absorptive_TA_1 PI3 2.873 3.95E−51 1.17E+00 8.61E−04 0.989 E.Absorptive_TA_1 REG4 3.493 3.77E−48 2.00E+00 3.91E−04 1.910 E.Absorptive_TA_1 RPL13A −1.230 1.49E−06 −6.81E−01  1.08E−19 −1.944 E.Absorptive_TA_1 RPL15 −1.123 3.27E−12 −6.16E−01  1.90E−14 −1.623 E.Absorptive_TA_1 RPL8 −0.957 2.66E−06 −5.23E−01  8.97E−15 −0.952 E.Absorptive_TA_1 RPLP0 −1.399 4.40E−17 −4.28E−01  2.11E−08 −1.250 E.Absorptive_TA_1 RPS14 −1.078 2.20E−07 −6.92E−01  1.13E−20 −1.631 E.Absorptive_TA_1 RPS18 −1.506 2.37E−07 −6.14E−01  6.68E−15 −2.203 E.Absorptive_TA_1 RPS2 −1.112 1.30E−06 −7.95E−01  2.76E−20 −1.830 E.Absorptive_TA_1 RPS5 −1.200 1.11E−16 −3.71E−01  1.91E−06 −1.125 E.Absorptive_TA_1 S100A11 0.801 2.56E−11 7.99E−01 9.69E−18 0.902 E.Absorptive_TA_1 S100P 3.499 7.00E−64 5.73E−01 5.27E−02 0.608 E.Absorptive_TA_1 SAA1 4.759 1.88E−19 1.00E+00 3.487 E.Absorptive_TA_2 AC009501.4 −2.035 1.89E−46 4.32E−01 8.41E−06 −1.587 E.Absorptive_TA_2 ARPC1B 0.803 8.00E−06 6.70E−01 9.84E−23 0.861 E.Absorptive_TA_2 ATP6V1G1 0.696 1.44E−04 7.10E−01 1.93E−30 0.590 E.Absorptive_TA_2 CD44 1.225 3.74E−14 8.89E−01 2.59E−18 0.827 E.Absorptive_TA_2 CXCL1 2.030 4.68E−21 1.74E+00 7.62E−09 0.740 E.Absorptive_TA_2 FAM3B −4.763 3.39E−26 1.00E+00 5.362 E.Absorptive_TA_2 FOS −2.217 1.09E−33 3.52E−01 1.33E−03 −1.065 E.Absorptive_TA_2 GPX2 1.975 1.93E−06 1.18E+00 4.04E−59 0.988 E.Absorptive_TA_2 IFITM3 0.713 3.27E−05 1.14E+00 1.16E−33 0.780 E.Absorptive_TA_2 JUN −2.140 1.07E−30 2.13E−01 2.99E−02 −0.715 E.Absorptive_TA_2 KRT19 1.926 6.67E−05 1.04E+00 1.44E−24 2.057 E.Absorptive_TA_2 LGALS4 −2.052 2.94E−03 −8.31E−01  7.58E−21 −1.057 E.Absorptive_TA_2 MUC12 2.943 6.71E−55 1.60E+00 2.73E−82 1.962 E.Absorptive_TA_2 OLFM4 2.263 2.18E−47 1.43E+00 8.82E−21 0.912 E.Absorptive_TA_2 PARP8 4.359 6.47E−27 1.00E+00 5.362 E.Absorptive_TA_2 PDIA3 1.138 2.14E−07 9.74E−01 1.53E−58 0.682 E.Absorptive_TA_2 PI3 2.532 4.68E−55 2.03E+00 3.86E−22 1.026 E.Absorptive_TA_2 PITX2 −5.183 2.15E−36 1.00E+00 5.362 E.Absorptive_TA_2 PLA2G2A 2.672 1.34E−35 2.35E+00  9.57E−124 1.526 E.Absorptive_TA_2 PRAC1 4.172  1.17E−107 6.60E−01 1.16E−14 0.845 E.Absorptive_TA_2 PSMB9 0.727 2.84E−06 8.15E−01 9.01E−28 0.702 E.Absorptive_TA_2 PSME2 0.656 5.51E−02 6.36E−01 2.68E−24 0.539 E.Absorptive_TA_2 REG4 2.978 5.55E−59 1.41E+00 1.65E−06 1.499 E.Absorptive_TA_2 RNASE1 1.197 5.71E−13 8.73E−01 1.38E−22 0.518 E.Absorptive_TA_2 RP11-708H21.4 −5.510 1.52E−35 1.00E+00 5.362 E.Absorptive_TA_2 RPS20 −2.005 5.54E−05 6.04E−01 1.49E−17 −1.030 E.Absorptive_TA_2 S100A10 0.724 4.05E−01 7.44E−01 1.05E−21 0.965 E.Absorptive_TA_2 S100A11 1.708 2.98E−07 1.34E+00 2.00E−79 2.043 E.Absorptive_TA_2 S100A6 0.806 6.47E−01 9.97E−01 1.50E−24 1.526 E.Absorptive_TA_2 S100A9 3.719 7.49E−29 1.11E+00 1.42E−01 0.636 E.Absorptive_TA_2 S100P 4.775  7.32E−142 1.82E+00 9.71E−41 2.118 E.Absorptive_TA_2 7-Sep 0.806 1.11E−07 7.46E−01 4.33E−22 0.521 E.Absorptive_TA_2 SH3BGRL3 0.384 2.41E−01 7.49E−01 1.17E−24 0.694 E.Absorptive_TA_2 SOD3 1.752 2.49E−26 1.22E+00 5.87E−19 1.117 E.Absorptive_TA_2 SSR4 1.419 4.08E−05 6.51E−01 2.25E−21 1.212 E.Absorptive_TA_2 ST3GAL4 2.321 1.54E−21 7.09E−01 1.95E−04 0.503 E.Absorptive_TA_2 ST6GALNAC6 2.484 1.09E−44 7.02E−01 1.02E−13 0.740 E.Best4_Enterocytes AC009501.4 −2.044 3.27E−22 4.88E−01 1.47E−02 −1.532 E.Best4_Enterocytes AQP8 −2.602 1.40E−28 1.56E−01 7.08E−01 −0.517 E.Best4_Enterocytes ARF4 1.190 3.64E−05 8.83E−01 1.07E−19 0.584 E.Best4_Enterocytes EIF4G2 1.075 2.23E−04 9.59E−01 5.21E−27 0.515 E.Best4_Enterocytes ITM2B 1.023 8.35E−03 1.05E+00 2.50E−21 1.406 E.Best4_Enterocytes LAPTM4A 0.907 4.12E−03 1.03E+00 9.39E−21 0.701 E.Best4_Enterocytes MT-ND4L 1.168 1.29E−04 1.06E+00 3.28E−29 0.614 E.Best4_Enterocytes MUC12 1.802 3.33E−09 1.07E+00 2.31E−19 0.784 E.Best4_Enterocytes RPL37 0.400 3.34E−01 1.03E+00 3.93E−20 0.714 E.Best4_Enterocytes RPL38 0.517 2.06E−01 9.36E−01 3.81E−20 0.648 E.Best4_Enterocytes RPL39 0.270 3.66E−01 2.26E+00 6.86E−40 0.567 E.Best4_Enterocytes S100A11 1.141 3.66E−04 1.32E+00 1.10E−30 1.492 E.Cycling_TA AK1 2.364 2.05E−47 5.53E−01 1.75E−09 0.894 E.Cycling_TA ANXA5 0.741 1.64E−07 8.29E−01 2.42E−27 0.569 E.Cycling_TA ARPC1B 0.754 4.22E−05 1.10E+00 2.61E−63 0.987 E.Cycling_TA C2 2.248 1.79E−22 1.01E+00 4.50E−09 0.707 E.Cycling_TA CAPG 0.852 1.98E−06 8.04E−01 1.75E−39 0.507 E.Cycling_TA CLDN2 4.506 2.72E−21 1.00E+00 5.347 E.Cycling_TA DDX5 0.446 4.03E−02 8.98E−01 1.59E−41 0.588 E.Cycling_TA DUOXA2 4.748 3.48E−46 1.70E+00 1.72E−01 0.584 E.Cycling_TA ENO1 1.107 8.45E−03 9.17E−01 1.33E−59 0.925 E.Cycling_TA FAM3B −4.685 2.85E−25 1.00E+00 5.347 E.Cycling_TA FN1 3.408 5.62E−29 1.26E+00 9.56E−03 1.190 E.Cycling_TA H3F3B 1.033 1.94E−02 7.37E−01 1.81E−26 1.500 E.Cycling_TA HLA-DMA 1.344 6.68E−20 1.22E+00 2.89E−27 0.881 E.Cycling_TA HLA-DRB1 1.673 5.80E−31 2.18E+00 1.38E−35 2.587 E.Cycling_TA HSPA5 1.222 7.03E−10 9.93E−01 1.89E−56 0.944 E.Cycling_TA IFI16 1.535 4.03E−16 8.25E−01 5.72E−11 0.564 E.Cycling_TA IFITM3 0.709 9.80E−04 1.29E+00 1.05E−52 0.800 E.Cycling_TA JUN −1.938 2.62E−20 6.40E−02 4.41E−01 −0.685 E.Cycling_TA LDHA 0.582 4.22E−02 9.94E−01 8.79E−58 0.557 E.Cycling_TA LYZ 1.419 4.50E−19 1.08E+00 2.71E−07 0.824 E.Cycling_TA MMP7 4.756 2.07E−20 1.00E+00 5.347 E.Cycling_TA MTRNR2L1 1.059 7.81E−16 1.00E+00 4.48E−09 1.035 E.Cycling_TA MUC12 2.558 1.09E−34 1.34E+00 2.06E−78 1.307 E.Cycling_TA PDIA3 1.005 2.85E−04 1.12E+00 2.93E−88 0.712 E.Cycling_TA PI3 1.750 2.09E−26 2.36E+00 1.06E−25 0.573 E.Cycling_TA PITX1 3.389 2.83E−33 5.86E−01 3.64E−02 1.746 E.Cycling_TA PITX2 −5.266 3.04E−38 1.00E+00 5.347 E.Cycling_TA PLA2G2A 2.181 6.66E−23 2.00E+00  3.70E−108 1.037 E.Cycling_TA PRAC1 4.338  1.08E−106 5.88E−01 1.59E−13 0.933 E.Cycling_TA PSMB9 0.574 7.69E−04 1.11E+00 1.52E−66 0.671 E.Cycling_TA PSME2 0.840 3.36E−02 1.01E+00 3.67E−64 0.783 E.Cycling_TA REG4 3.108 3.27E−91 2.18E+00 1.61E−22 2.029 E.Cycling_TA RPL36AL 0.535 2.03E−01 7.16E−01 1.81E−43 0.691 E.Cycling_TA RPL38 −1.396 1.21E−03 6.04E−01 5.50E−24 −0.518 E.Cycling_TA S100A10 0.542 3.09E−01 6.87E−01 7.21E−20 0.728 E.Cycling_TA S100A11 1.278 1.93E−05 1.48E+00  9.57E−108 1.704 E.Cycling_TA S100P 4.483  2.51E−135 1.53E+00 3.04E−29 1.934 E.Cycling_TA SAA1 4.886 3.06E−38 1.00E+00 5.347 E.Cycling_TA SH3BGRL3 0.466 2.04E−01 9.51E−01 4.79E−42 0.896 E.Cycling_TA SPCS1 0.997 1.14E−03 7.51E−01 2.22E−49 0.702 E.Cycling_TA ST6GALNAC6 2.373 5.30E−36 7.72E−01 1.53E−11 0.641 E.Cycling_TA TESC 3.977 5.68E−31 7.30E−01 1.78E−01 1.524 E.Cycling_TA UBL5 0.763 4.90E−02 7.22E−01 7.05E−46 0.562 E.Enterocyte_Immature_1 AC009501.4 −1.578 1.07E−27 4.98E−01 4.99E−05 −1.207 E.Enterocyte_Immature_1 MUC1 2.225 1.32E−28 1.25E+00 9.20E−14 0.989 E.Enterocyte_Immature_1 MUC4 2.580 1.36E−27 1.01E+00 7.66E−10 0.648 E.Enterocyte_Immature_1 OAZ1 −0.919 2.43E−06 −5.61E−01  4.55E−15 −0.526 E.Enterocyte_Immature_1 PLA2G2A 3.060 8.53E−55 1.01E+00 2.00E−04 1.432 E.Enterocyte_Immature_1 RNASE1 1.506 1.12E−19 7.19E−01 2.15E−06 0.652 E.Enterocyte_Immature_1 S100P 3.636 1.24E−50 1.18E+00 3.28E−04 0.858 E.Enterocyte_Immature_1 TNIP3 4.533 1.08E−18 1.00E+00 3.737 E.Enterocyte_Immature_1 XIST 1.241 2.78E−11 9.86E−01 6.99E−12 0.558 E.Enterocyte_Immature_2 AC009501.4 −2.768 2.25E−73 3.42E−01 6.64E−03 −1.914 E.Enterocyte_Immature_2 AGR2 1.354 2.45E−08 1.63E+00 3.94E−52 1.375 E.Enterocyte_Immature_2 AQP8 −2.453 1.34E−53 −1.12E+00  4.78E−09 −0.542 E.Enterocyte_Immature_2 BHLHE40 2.162 3.21E−25 7.35E−01 3.35E−08 0.747 E.Enterocyte_Immature_2 CCL20 2.820 5.35E−24 2.45E+00 5.30E−09 0.855 E.Enterocyte_Immature_2 CEACAM5 1.784 6.07E−09 1.20E+00 3.93E−42 1.233 E.Enterocyte_Immature_2 CEACAM6 1.929 1.16E−34 1.13E+00 1.89E−36 0.560 E.Enterocyte_Immature_2 CLIC3 2.244 5.14E−20 8.02E−01 3.27E−05 0.515 E.Enterocyte_Immature_2 CRIP1 1.028 3.37E−11 7.47E−01 1.57E−25 0.637 E.Enterocyte_Immature_2 CTSE 3.988 1.76E−39 9.98E−01 2.51E−02 0.948 E.Enterocyte_Immature_2 CXCL1 3.232 4.63E−31 2.99E+00 2.20E−08 1.874 E.Enterocyte_Immature_2 CXCL2 2.355 1.36E−17 1.83E+00 1.06E−07 0.796 E.Enterocyte_Immature_2 DDX5 0.541 5.23E−03 7.54E−01 1.97E−23 0.608 E.Enterocyte_Immature_2 FAM3C 1.790 9.09E−23 7.90E−01 1.03E−14 0.504 E.Enterocyte_Immature_2 FOSB −2.318 3.62E−41 8.57E−02 3.99E−01 −0.563 E.Enterocyte_Immature_2 FTL −1.369 4.53E−02 −9.90E−01  5.23E−26 −1.925 E.Enterocyte_Immature_2 GPX2 1.336 1.26E−13 1.58E+00 2.45E−62 0.700 E.Enterocyte_Immature_2 HSPA5 0.720 3.48E−05 1.16E+00 4.47E−47 0.566 E.Enterocyte_Immature_2 HSPB1 −1.098 2.00E−04 −8.02E−01  3.51E−22 −0.552 E.Enterocyte_Immature_2 IL2RG 1.424 3.34E−22 6.95E−01 2.30E−18 1.183 E.Enterocyte_Immature_2 MDK 1.022 1.38E−10 6.62E−01 6.49E−12 0.506 E.Enterocyte_Immature_2 MUC12 2.103 1.06E−18 1.75E+00  1.24E−108 1.048 E.Enterocyte_Immature_2 PDIA3 0.832 2.28E−05 8.17E−01 3.32E−34 0.527 E.Enterocyte_Immature_2 PITX2 −5.108 9.63E−37 1.00E+00 4.699 E.Enterocyte_Immature_2 PLA2G2A 3.223 1.25E−74 2.16E+00 1.22E−52 2.024 E.Enterocyte_Immature_2 RARRES3 1.373 2.76E−20 8.93E−01 1.94E−24 1.463 E.Enterocyte_Immature_2 RNASE1 1.490 3.23E−18 9.83E−01 8.18E−21 0.722 E.Enterocyte_Immature_2 S100A11 2.296 1.40E−34 1.73E+00 4.50E−84 3.042 E.Enterocyte_Immature_2 S100A6 0.487 8.95E−01 1.22E+00 1.13E−33 1.347 E.Enterocyte_Immature_2 S100A9 4.778 1.09E−35 1.00E+00 4.699 E.Enterocyte_Immature_2 S100P 4.403  5.49E−119 2.48E+00 1.80E−93 2.215 E.Enterocyte_Immature_2 SAA1 4.632 2.47E−25 1.00E+00 4.699 E.Enterocyte_Immature_2 SDCBP 1.046 2.94E−11 8.86E−01 2.61E−28 0.730 E.Enterocyte_Immature_2 SEC24D 3.545 1.92E−21 7.11E−01 1.14E−01 0.740 E.Enterocyte_Immature_2 SEPP1 1.501 5.03E−16 1.06E+00 6.71E−25 1.821 E.Enterocyte_Immature_2 SERPINB5 4.888 2.54E−29 1.00E+00 4.699 E.Enterocyte_Immature_2 SLC6A14 4.678 1.75E−25 1.00E+00 4.699 E.Enterocyte_Immature_2 TFF1 2.726 2.86E−65 1.43E+00 2.79E−19 1.847 E.Enterocyte_Immature_2 TIMP2 1.921 1.69E−15 6.59E−01 1.42E−05 0.648 E.Enterocyte_Immature_2 TNIP3 4.989 2.93E−32 1.00E+00 4.699 E.Enterocyte_Immature_2 TPM4 1.104 8.57E−11 6.95E−01 6.54E−26 0.528 E.Enterocyte_Immature_2 TRAM1 1.156 5.21E−12 7.44E−01 2.20E−18 0.621 E.Enterocyte_Progenitor AC009501.4 −1.790 4.78E−28 8.23E−01 1.42E−07 −1.363 E.Enterocyte_Progenitor AGR2 0.874 2.18E−07 1.07E+00 7.14E−15 0.618 E.Enterocyte_Progenitor CCL20 3.364 7.51E−25 9.45E−01 5.44E−02 0.971 E.Enterocyte_Progenitor CEACAM5 1.304 1.77E−16 1.11E+00 4.55E−19 0.797 E.Enterocyte_Progenitor CEACAM6 2.165 4.16E−21 1.25E+00 2.50E−09 0.725 E.Enterocyte_Progenitor CXCL1 3.601 2.78E−26 1.55E+00 2.06E−02 2.451 E.Enterocyte_Progenitor CXCL3 2.597 3.47E−20 1.69E+00 2.00E−06 0.832 E.Enterocyte_Progenitor DUOXA2 5.301 6.59E−34 1.00E+00 4.362 E.Enterocyte_Progenitor GPX2 1.489 2.06E−20 1.17E+00 7.68E−23 0.648 E.Enterocyte_Progenitor HSPB1 −1.810 3.57E−27 −3.83E−01  2.31E−03 −0.614 E.Enterocyte_Progenitor LCN2 2.265 4.40E−38 2.19E+00 1.65E−28 0.771 E.Enterocyte_Progenitor OLFM4 2.962 6.59E−34 1.43E+00 2.90E−05 1.256 E.Enterocyte_Progenitor PI3 2.248 6.99E−37 2.35E+00 3.39E−25 0.698 E.Enterocyte_Progenitor PLA2G2A 2.744 4.26E−57 1.65E+00 8.27E−20 1.295 E.Enterocyte_Progenitor S100A11 1.487 1.34E−20 1.16E+00 5.79E−25 1.808 E.Enterocyte_Progenitor S100A6 1.420 2.81E−01 1.21E+00 5.11E−27 2.188 E.Enterocyte_Progenitor S100A9 4.821 1.22E−24 1.00E+00 4.362 E.Enterocyte_Progenitor S100P 4.217  7.74E−100 1.40E+00 3.88E−11 1.481 E.Enterocyte_Progenitor TFF1 2.396 4.72E−26 1.24E+00 2.37E−04 1.400 E.Enterocyte_Progenitor TNIP3 4.724 2.35E−19 1.00E+00 4.362 E.Enterocyte_Progenitor TPT1 0.631 1.65E−03 7.81E−01 1.21E−19 0.944 E.Enterocytes AC009501.4 −2.349 9.38E−52 5.09E−01 3.37E−05 −1.707 E.Enterocytes BHLHE40 2.112 1.35E−30 7.65E−01 1.16E−10 0.777 E.Enterocytes C4orf3 1.121 3.18E−11 9.20E−01 7.30E−34 0.869 E.Enterocytes CA2 −2.970 9.81E−18 −1.13E+00  4.28E−27 −0.602 E.Enterocytes CARD16 0.989 5.33E−08 1.40E+00 2.00E−33 0.754 E.Enterocytes CASP1 1.981 1.44E−22 1.42E+00 1.62E−24 1.256 E.Enterocytes CCNJL −4.668 5.35E−22 1.00E+00 5.613 E.Enterocytes CD55 1.595 2.02E−21 1.36E+00 4.01E−34 0.776 E.Enterocytes CTSE 3.644 7.81E−41 1.38E+00 1.03E−04 0.623 E.Enterocytes CXCL1 3.416 1.52E−39 2.76E+00 2.35E−07 2.315 E.Enterocytes CXCL3 2.170 4.29E−24 2.21E+00 5.65E−16 0.668 E.Enterocytes FSTL1 4.180 4.28E−21 1.00E+00 5.613 E.Enterocytes FTH1 0.338 8.97E−01 −1.26E+00  5.68E−33 −0.744 E.Enterocytes GLDN 4.849 1.07E−29 1.00E+00 5.613 E.Enterocytes GLUL 1.393 2.71E−11 1.29E+00 2.02E−15 0.668 E.Enterocytes GPX2 1.242 1.22E−11 2.19E+00 2.23E−47 0.744 E.Enterocytes GPX4 −2.068 3.20E−22 −4.83E−01  1.02E−11 −0.516 E.Enterocytes GUCA2A −4.568 4.77E−31 −8.72E−01  2.27E−11 −0.540 E.Enterocytes HLA-B 1.277 3.56E−01 8.45E−01 5.24E−23 2.037 E.Enterocytes HLA-F 1.058 2.46E−10 7.24E−01 4.55E−27 0.529 E.Enterocytes IDO1 4.493 2.75E−27 1.00E+00 5.613 E.Enterocytes IFITM3 1.886 4.92E−26 1.91E+00 2.31E−23 2.733 E.Enterocytes IL2RG 0.819 4.99E−07 8.66E−01 1.06E−32 0.645 E.Enterocytes ITM2B 0.372 1.66E−01 9.06E−01 1.02E−27 0.602 E.Enterocytes KDELR3 3.122 1.27E−19 7.14E−01 4.43E−02 0.587 E.Enterocytes LAPTM4A 0.767 2.50E−05 8.99E−01 1.91E−24 0.575 E.Enterocytes LPCAT1 3.289 9.48E−23 4.78E−01 1.42E−01 0.543 E.Enterocytes MARCKSL1 1.542 2.40E−17 7.01E−01 1.60E−16 0.785 E.Enterocytes MMP7 4.672 5.17E−23 1.00E+00 5.613 E.Enterocytes MUC1 1.629 4.62E−20 1.45E+00 4.47E−35 0.630 E.Enterocytes OLFM4 2.237 6.26E−23 1.76E+00 1.51E−08 0.670 E.Enterocytes PFKFB3 3.265 3.75E−34 9.27E−01 2.44E−04 1.121 E.Enterocytes PITX2 −5.485 2.67E−47 1.00E+00 5.613 E.Enterocytes PKM 0.850 3.61E−06 1.44E+00 6.67E−61 0.716 E.Enterocytes PLA2G16 1.790 2.78E−18 7.22E−01 2.02E−06 0.863 E.Enterocytes PLA2G2A 2.920 9.64E−57 2.21E+00 4.22E−24 1.774 E.Enterocytes PNRC1 0.761 1.47E−06 8.21E−01 1.00E−18 0.645 E.Enterocytes PSMB9 0.428 1.26E−02 1.05E+00 4.20E−44 0.502 E.Enterocytes PSME2 1.196 8.23E−06 1.13E+00 3.69E−54 1.201 E.Enterocytes RARRES3 2.176 1.34E−22 1.02E+00 2.51E−48 2.320 E.Enterocytes REG4 3.497 2.26E−36 1.99E+00 3.33E−03 2.049 E.Enterocytes RNASE1 1.914 3.26E−29 1.36E+00 3.41E−27 1.372 E.Enterocytes S100A11 2.028 4.04E−28 2.69E+00 7.68E−72 3.482 E.Enterocytes S100A9 4.819 1.77E−36 1.00E+00 5.613 E.Enterocytes S100P 2.774 8.64E−45 1.83E+00 2.45E−21 0.527 E.Enterocytes SERPINB5 4.782 2.34E−28 1.00E+00 5.613 E.Enterocytes SLC6A14 4.958 2.33E−32 1.00E+00 5.613 E.Enterocytes SOCS1 1.172 1.49E−10 1.45E+00 2.99E−26 0.654 E.Enterocytes SRI −1.855 1.09E−03 −7.90E−01  8.80E−24 −0.511 E.Enterocytes TC2N 2.673 1.04E−24 6.58E−01 1.36E−03 0.608 E.Enterocytes TFF1 1.694 2.24E−24 1.78E+00 6.57E−38 0.631 E.Enterocytes TNIP3 4.597 1.38E−38 1.96E+00 4.96E−02 0.752 E.Enterocytes UBE2L6 1.501 2.38E−17 6.19E−01 8.51E−09 0.885 E.Enterocytes VAMP5 1.397 6.09E−19 7.76E−01 2.78E−12 1.132 E.Enterocytes WARS 1.943 5.03E−16 1.11E+00 4.93E−08 0.904 E.Epithelial AC009501.4 −1.443  7.79E−132 4.72E−01 6.10E−31 −1.149 E.Epithelial ANXA1 1.532 1.71E−21 9.34E−01 5.59E−05 2.273 E.Epithelial C2 2.419 4.00E−35 4.07E−01 2.16E−02 0.718 E.Epithelial CLDN2 4.210 6.55E−22 1.00E+00 3.712 E.Epithelial CLIC3 1.511 2.81E−16 7.55E−01 5.91E−06 0.730 E.Epithelial CLU 1.765 3.90E−24 4.83E−01 2.92E−02 0.713 E.Epithelial CXCL1 2.124 3.72E−61 1.59E+00 4.85E−12 0.799 E.Epithelial CXCL14 −0.977 1.47E−43 2.74E−01 1.18E−02 −0.638 E.Epithelial DAPP1 3.360 3.08E−22 6.57E−01 3.29E−01 0.689 E.Epithelial DDX5 0.586 1.04E−15 5.38E−01 2.57E−53 0.735 E.Epithelial DUSP1 −0.762 4.30E−29 1.82E−01 1.58E−04 −0.600 E.Epithelial EMB 2.867 8.44E−25 4.77E−01 2.03E−01 1.071 E.Epithelial FN1 2.696 7.40E−24 1.01E+00 1.27E−02 0.755 E.Epithelial FOS −0.854 5.67E−35 −3.32E−02  4.67E−01 −0.748 E.Epithelial FTL −0.865 1.12E−11 −6.64E−01  1.34E−65 −1.441 E.Epithelial FYB 1.577 3.28E−24 3.85E−01 9.34E−03 1.069 E.Epithelial GNB2L1 −0.865 6.70E−21 −3.72E−01  1.89E−29 −1.038 E.Epithelial HLA-DMA 1.393 9.54E−48 6.45E−01 1.16E−13 0.980 E.Epithelial HLA-DMB 1.558 1.95E−21 3.37E−01 3.23E−02 0.699 E.Epithelial HLA-DRB5 0.896 2.04E−19 7.32E−01 5.36E−10 0.744 E.Epithelial HLA-E 0.299 1.23E−05 4.98E−01 1.09E−47 0.503 E.Epithelial HOXD13 4.124 7.08E−25 1.00E+00 3.712 E.Epithelial IFI16 1.281 9.80E−16 5.37E−01 5.23E−06 0.583 E.Epithelial IFITM2 0.683 9.63E−14 4.51E−01 5.34E−09 0.863 E.Epithelial IL2RG 1.125 7.11E−55 5.06E−01 3.53E−20 1.076 E.Epithelial JUN −1.096 7.03E−55 −1.23E−01  2.44E−03 −0.544 E.Epithelial LYZ 1.686 3.73E−65 7.01E−01 2.11E−05 1.159 E.Epithelial MMP7 4.672 5.73E−32 1.00E+00 3.712 E.Epithelial MTRNR2L1 0.769 2.37E−35 1.50E+00 1.88E−65 0.583 E.Epithelial MYL6 −0.723 1.96E−08 −2.21E−01  7.35E−14 −0.543 E.Epithelial NPSR1 4.209 1.31E−20 1.00E+00 3.712 E.Epithelial PARP8 3.281 5.72E−27 5.60E−01 2.18E−01 1.215 E.Epithelial PDIA3 0.781 9.84E−26 7.38E−01  9.60E−107 0.577 E.Epithelial PITX1 3.327 1.93E−29 5.18E−01 2.50E−01 1.404 E.Epithelial PLA2G16 1.312 6.03E−16 5.71E−01 3.33E−05 0.818 E.Epithelial RARRES3 0.983 5.05E−46 5.61E−01 1.35E−26 1.172 E.Epithelial RBPMS 3.215 8.44E−25 8.90E−01 8.58E−02 1.970 E.Epithelial RPL10A −0.494 4.20E−10 −2.63E−01  3.96E−12 −0.638 E.Epithelial RPL11 −0.604 4.93E−07 −3.64E−01  4.47E−29 −0.840 E.Epithelial RPL12 −0.703 4.84E−12 −3.45E−01  3.32E−22 −0.949 E.Epithelial RPL15 −0.607 3.55E−11 −4.52E−01  6.87E−36 −0.808 E.Epithelial RPL3 −0.432 2.77E−05 −3.97E−01  1.04E−27 −0.599 E.Epithelial RPL8 −0.453 1.38E−04 −4.33E−01  2.01E−42 −0.754 E.Epithelial RPLP0 −0.670 5.02E−14 −3.92E−01  3.93E−27 −0.893 E.Epithelial RPS14 −0.714 5.62E−09 −5.30E−01  4.82E−55 −1.072 E.Epithelial RPS3 −0.562 8.06E−07 −5.03E−01  6.89E−46 −0.920 E.Epithelial RPS4X −0.747 3.99E−15 −3.57E−01  4.14E−22 −0.793 E.Epithelial RPS5 −0.778 1.04E−18 −4.38E−01  2.13E−34 −1.056 E.Epithelial RPS6 −0.345 1.94E−03 −4.07E−01  4.67E−25 −0.516 E.Epithelial RPS7 −0.553 1.08E−10 −2.31E−01  3.16E−11 −0.722 E.Epithelial RPS8 −0.421 1.64E−06 −2.92E−01  1.81E−14 −0.608 E.Epithelial RPS9 −0.499 6.83E−07 −3.42E−01  6.59E−25 −0.724 E.Epithelial S100A11 1.027 3.60E−50 1.14E+00  5.42E−174 1.438 E.Epithelial S100A6 0.316 2.20E−01 9.80E−01  7.47E−166 0.766 E.Epithelial S100A9 3.465 6.87E−51 1.36E+00 1.54E−02 0.852 E.Epithelial SEPP1 0.517 9.21E−18 6.80E−01 1.65E−25 0.513 E.Epithelial SLC25A6 −0.922 1.36E−28 −3.28E−01  2.06E−25 −0.505 E.Epithelial SLC6A14 4.840 3.60E−45 1.00E+00 3.712 E.Epithelial SOCS1 1.303 5.89E−25 9.77E−01 4.12E−19 1.015 E.Epithelial SOD3 1.247 7.61E−45 6.69E−01 1.58E−17 0.526 E.Epithelial TESC 3.086 1.80E−29 −1.68E−01  6.55E−01 0.938 E.Epithelial TGFBI 2.541 1.53E−24 5.92E−01 4.34E−02 1.252 E.Epithelial TGM2 3.983 1.26E−26 1.00E+00 3.712 E.Epithelial TIMP1 2.832  3.53E−214 7.38E−01 1.84E−09 2.805 E.Epithelial TNIP3 4.624 1.56E−50 1.00E+00 3.712 E.Goblet CD55 1.848 2.06E−17 5.48E−01 4.68E−04 0.782 E.Goblet REG4 2.119 7.02E−31 1.68E+00 2.41E−14 0.585 E.Immature_Enterocytes AC009501.4 −1.996  2.17E−109 4.73E−01 9.38E−10 −1.467 E.Immature_Enterocytes ACTB 0.736 5.40E−03 4.95E−01 2.53E−18 1.195 E.Immature_Enterocytes AGR2 0.813 2.93E−16 1.11E+00 2.45E−51 0.652 E.Immature_Enterocytes ATP5G2 −1.021 3.18E−20 −1.40E−01  9.24E−03 −0.522 E.Immature_Enterocytes BHLHE40 1.813 1.08E−28 6.05E−01 8.32E−08 0.533 E.Immature_Enterocytes C2 3.396 1.06E−23 6.41E−01 1.22E−01 1.513 E.Immature_Enterocytes CCL20 2.626 2.55E−53 1.72E+00 4.25E−13 0.694 E.Immature_Enterocytes CD55 1.431 4.60E−29 7.57E−01 8.67E−18 0.528 E.Immature_Enterocytes COX4I1 −0.986 1.64E−10 −6.32E−01  5.86E−41 −0.656 E.Immature_Enterocytes CTSE 3.705 4.13E−51 7.71E−01 2.08E−02 0.720 E.Immature_Enterocytes CXCL1 3.293 1.44E−60 1.96E+00 6.03E−07 2.170 E.Immature_Enterocytes CXCL2 2.244 3.20E−26 1.52E+00 6.15E−09 0.717 E.Immature_Enterocytes CXCL3 1.917 8.57E−32 2.03E+00 9.47E−24 0.675 E.Immature_Enterocytes DDX5 0.668 1.49E−11 5.71E−01 2.49E−26 0.688 E.Immature_Enterocytes FABP1 −3.053 1.37E−11 −4.59E−01  3.65E−10 −0.930 E.Immature_Enterocytes FSTL1 3.298 1.82E−20 9.38E−01 2.20E−02 1.375 E.Immature_Enterocytes FTL −0.984 2.24E−07 −8.67E−01  1.10E−47 −1.585 E.Immature_Enterocytes GLRA2 4.429 1.50E−22 1.00E+00 3.780 E.Immature_Enterocytes GPX2 1.284 7.15E−38 1.34E+00 1.93E−78 0.727 E.Immature_Enterocytes GSN 0.622 2.20E−11 5.12E−01 6.60E−17 0.566 E.Immature_Enterocytes H3F3B 0.379 1.83E−03 4.65E−01 1.29E−20 0.648 E.Immature_Enterocytes HLA-DMA 1.146 1.05E−14 7.23E−01 2.28E−07 0.629 E.Immature_Enterocytes HLA-DRB1 1.115 5.71E−32 8.99E−01 2.54E−16 1.133 E.Immature_Enterocytes IFITM3 0.996 1.88E−17 1.21E+00 1.10E−24 1.235 E.Immature_Enterocytes IL2RG 1.050 2.54E−29 4.06E−01 1.21E−11 0.680 E.Immature_Enterocytes LCN2 1.652 5.00E−55 2.28E+00 2.32E−81 0.630 E.Immature_Enterocytes MUC12 1.575 2.63E−52 1.49E+00  5.82E−173 0.507 E.Immature_Enterocytes MYL6 −1.070 8.96E−08 −3.39E−01  2.58E−14 −0.809 E.Immature_Enterocytes PARP8 4.286 2.54E−27 1.00E+00 3.780 E.Immature_Enterocytes PITX2 −5.336 1.15E−51 1.00E+00 3.780 E.Immature_Enterocytes PLA2G2A 2.792  1.36E−159 1.74E+00 1.05E−55 1.666 E.Immature_Enterocytes PPDPF −0.764 4.22E−07 −4.13E−01  7.60E−19 −0.573 E.Immature_Enterocytes RARRES3 1.072 9.26E−31 5.27E−01 3.33E−18 0.946 E.Immature_Enterocytes REG4 2.421 2.29E−41 1.33E+00 3.34E−05 0.904 E.Immature_Enterocytes RNASE1 1.291 2.61E−34 8.99E−01 1.66E−28 0.679 E.Immature_Enterocytes S100A11 1.519 2.59E−54 1.36E+00 1.34E−88 2.079 E.Immature_Enterocytes S100A6 2.704 1.21E−03 9.85E−01 3.00E−65 2.484 E.Immature_Enterocytes S100A9 5.071 3.74E−55 1.00E+00 3.780 E.Immature_Enterocytes S100P 3.659  2.13E−223 2.01E+00 8.60E−74 1.180 E.Immature_Enterocytes SDCBP 0.829 1.54E−15 6.27E−01 4.94E−22 0.519 E.Immature_Enterocytes SEC24D 3.280 1.34E−28 5.32E−01 6.92E−02 0.541 E.Immature_Enterocytes SEPP1 1.092 5.01E−32 7.78E−01 7.85E−29 1.165 E.Immature_Enterocytes SLC25A6 −1.100 2.75E−22 −4.08E−01  2.29E−16 −0.552 E.Immature_Enterocytes SLC6A14 4.944 1.67E−36 1.00E+00 3.780 E.Immature_Enterocytes SOCS1 1.505 5.40E−20 1.04E+00 2.25E−15 0.930 E.Immature_Enterocytes SPINK1 0.967 9.15E−18 1.72E+00 8.72E−61 0.613 E.Immature_Enterocytes TFF1 2.048 8.47E−97 1.33E+00 4.98E−33 1.056 E.Immature_Enterocytes TGM2 3.379 1.71E−20 1.33E+00 3.61E−03 0.737 E.Immature_Enterocytes TNIP3 5.326 4.69E−59 1.00E+00 3.780 E.Immature_Goblet AC009501.4 −1.337 4.88E−18 5.82E−01 3.69E−05 −1.044 E.Immature_Goblet CCL20 2.890 3.18E−19 8.86E−01 5.94E−02 0.727 E.Immature_Goblet COX4I1 −1.191 5.15E−05 −7.55E−01  6.18E−24 −0.820 E.Immature_Goblet RPL10 −1.902 2.44E−04 −7.44E−01  1.13E−17 −2.877 E.Immature_Goblet RPL8 −1.005 8.44E−03 −6.59E−01  2.58E−19 −1.040 E.Immature_Goblet S100P 3.344 8.37E−84 1.23E+00 1.13E−19 0.534 E.Immature_Goblet TFF1 2.786 6.36E−57 1.44E+00 6.23E−09 1.843 E.Immature_Goblet XIST 1.805 3.50E−20 6.50E−01 1.68E−05 0.796 E.Secretory CD55 1.774 1.22E−18 5.78E−01 5.94E−05 0.720 E.Secretory MT-ND3 0.612 2.87E−04 1.74E+00 1.68E−42 0.840 E.Secretory_All AC009501.4 −1.407 1.77E−55 2.10E−01 3.91E−03 −1.175 E.Secretory_All ANXA5 0.814 6.68E−15 3.89E−01 4.64E−08 0.500 E.Secretory_All C2 2.862 7.54E−34 5.68E−01 4.29E−03 0.984 E.Secretory_All C2CD4A 4.621 3.44E−22 1.00E+00 3.977 E.Secretory_All COX4I1 −1.041 3.46E−12 −6.80E−01  3.70E−51 −0.782 E.Secretory_All DDX5 0.746 3.77E−13 5.55E−01 2.80E−25 0.726 E.Secretory_All F3 2.004 6.47E−27 5.77E−01 1.18E−03 0.622 E.Secretory_All FN1 3.749 4.17E−30 1.04E+00 1.26E−01 1.293 E.Secretory_All GNB2L1 −0.763 2.24E−08 −4.37E−01  4.28E−18 −0.718 E.Secretory_All GSN 0.687 4.27E−12 5.83E−01 9.40E−19 0.760 E.Secretory_All HLA-E 0.552 2.99E−08 5.37E−01 8.98E−28 0.710 E.Secretory_All HSPB1 −0.997 2.07E−21 −1.16E−01  1.00E−01 −0.515 E.Secretory_All IGFALS 4.692 1.58E−22 1.00E+00 3.977 E.Secretory_All LGALS4 −0.832 9.78E−07 −6.12E−01  7.75E−26 −0.554 E.Secretory_All LYZ 2.134 6.69E−71 5.62E−01 1.37E−03 1.474 E.Secretory_All MTRNR2L1 0.697 1.03E−13 1.06E+00 5.67E−15 0.708 E.Secretory_All MUC5AC 4.738 1.60E−25 1.00E+00 3.977 E.Secretory_All MYL6 −0.771 2.97E−05 −3.64E−01  9.90E−17 −0.611 E.Secretory_All RARRES3 0.880 8.46E−18 3.05E−01 1.87E−05 0.671 E.Secretory_All RPL10 −0.754 6.30E−05 −5.97E−01  4.67E−25 −1.350 E.Secretory_All RPL11 −0.775 1.13E−05 −4.09E−01  2.73E−16 −1.037 E.Secretory_All RPL12 −0.637 3.49E−05 −4.50E−01  4.19E−17 −0.864 E.Secretory_All RPL13A −0.451 2.29E−02 −5.80E−01  8.75E−27 −0.905 E.Secretory_All RPL15 −0.448 1.20E−03 −5.43E−01  3.56E−21 −0.803 E.Secretory_All RPL8 −0.363 3.38E−02 −6.33E−01  4.82E−40 −0.616 E.Secretory_All RPLP0 −0.392 3.24E−03 −5.07E−01  4.81E−21 −0.541 E.Secretory_All RPS14 −0.703 4.32E−05 −5.44E−01  1.02E−24 −1.105 E.Secretory_All RPS2 −0.292 6.78E−02 −8.30E−01  1.92E−36 −0.895 E.Secretory_All RPS3 −0.460 6.04E−03 −6.15E−01  1.01E−29 −0.814 E.Secretory_All RPS5 −0.666 3.53E−07 −5.84E−01  4.59E−27 −0.790 E.Secretory_All RPS6 −0.440 1.61E−02 −5.67E−01  1.45E−21 −0.859 E.Secretory_All S100A11 0.648 2.98E−10 6.82E−01 8.40E−38 0.632 E.Secretory_All TESC 3.081 1.10E−26 −3.44E−01  2.63E−01 0.640 E.Secretory_All TGFBI 2.094 8.71E−26 4.21E−01 8.92E−03 0.906 E.Secretory_All TIMP1 2.353  1.54E−111 2.76E−01 1.43E−02 2.162 E.Secretory_All TRIM22 2.716 6.77E−21 4.84E−01 4.41E−02 0.720 E.Secretory_TA AC009501.4 −1.922 8.21E−33 3.93E−01 1.28E−03 −1.493 E.Secretory_TA AGR2 0.853 1.63E−01 1.34E+00 6.39E−32 0.743 E.Secretory_TA ATP6V1G1 0.927 1.17E−04 6.61E−01 1.05E−21 0.720 E.Secretory_TA CLDN2 4.820 2.51E−21 1.00E+00 5.000 E.Secretory_TA FN1 4.014 5.26E−30 1.24E+00 6.58E−02 1.790 E.Secretory_TA FRZB 1.444 1.41E−15 7.15E−01 2.96E−06 0.564 E.Secretory_TA HLA-F 1.278 9.14E−13 8.25E−01 1.00E−22 0.711 E.Secretory_TA HSPA5 0.707 3.67E−04 9.37E−01 6.96E−31 0.504 E.Secretory_TA ID3 −2.462 3.54E−33 1.86E−02 8.68E−01 −0.521 E.Secretory_TA IFITM3 0.474 3.08E−02 1.19E+00 5.35E−29 0.552 E.Secretory_TA MUC12 1.620 1.67E−15 1.00E+00 1.50E−27 0.560 E.Secretory_TA PDIA3 1.223 6.40E−06 8.66E−01 1.63E−36 0.820 E.Secretory_TA PI3 1.933 5.42E−20 1.40E+00 7.05E−07 0.511 E.Secretory_TA PITX2 −4.655 3.26E−22 1.00E+00 5.000 E.Secretory_TA PRAC1 3.889 7.68E−69 8.65E−01 8.21E−21 0.641 E.Secretory_TA PSMB9 0.578 1.62E−03 1.09E+00 3.57E−40 0.664 E.Secretory_TA REG4 2.058 5.48E−35 2.08E+00 8.85E−28 0.795 E.Secretory_TA S100A11 0.914 2.80E−03 9.52E−01 9.56E−31 1.044 E.Secretory_TA S100P 3.744 1.30E−76 1.55E+00 1.46E−27 1.083 E.Secretory_TA SAA1 4.764 3.13E−27 1.00E+00 5.000 E.Secretory_TA ST6GALNAC6 2.139 6.48E−23 6.58E−01 3.40E−08 0.504 E.Secretory_TA SUB1 0.866 1.14E−04 8.38E−01 1.60E−30 0.578 E.Secretory_TA TESC 4.021 2.87E−26 9.33E−01 7.33E−02 1.638 E.Stem PLA2G2A 2.205 3.62E−15 1.30E+00 8.28E−11 0.780 E.Stem PRAC1 4.659 1.44E−42 8.96E−01 4.25E−10 1.215 E.Stem WFDC2 1.916 8.85E−11 1.27E+00 4.00E−15 0.610 F.Crypt MME 4.670 1.98E−19 1.00E+00 1.880 F.Crypt MT-ND2 0.554 5.48E−03 7.23E−01 6.74E−18 1.118 F.Crypt MTRNR2L1 1.470 7.43E−23 1.35E+00 9.35E−11 1.524 F.Crypt NEAT1 0.816 8.97E−11 6.22E−01 2.99E−14 0.697 F.Crypt TAGLN 1.972 9.97E−40 7.73E−01 9.39E−06 0.919 F.Crypt_hiFos GSN −2.426 2.22E−11 −1.15E+00  1.94E−14 −0.619 F.Crypt_hiFos TAGLN 2.893 1.13E−27 7.76E−01 2.01E−02 1.916 F.Crypt_loFos_1 TAGLN 2.131 3.20E−18 8.60E−01 3.21E−03 1.061 F.Crypt_loFos_2 APOE −2.835 4.08E−17 −1.43E+00  8.91E−15 −0.785 F.Crypt_loFos_2 MTRNR2L1 2.610 1.48E−28 1.02E+00 6.59E−03 2.694 F.Endothelial AC005540.3 3.774 3.20E−22 5.85E−01 4.07E−01 0.660 F.Endothelial ANXA2 0.809 2.90E−09 1.02E+00 5.78E−45 0.721 F.Endothelial CD9 1.131 3.61E−20 3.90E−01 2.00E−05 1.049 F.Endothelial GAPDH 0.640 1.38E−03 5.31E−01 1.38E−17 0.754 F.Endothelial HLA-A −1.590 1.36E−06 −6.64E−01  1.04E−24 −1.462 F.Endothelial HLA-C −0.617 9.10E−02 −5.77E−01  5.04E−24 −0.617 F.Endothelial LGALS1 0.527 1.88E−05 8.46E−01 4.01E−19 1.028 F.Endothelial MTRNR2L1 2.205 8.01E−57 −6.75E−02  7.67E−01 1.668 F.Endothelial S100A6 0.691 5.92E−06 1.01E+00 2.42E−27 1.430 F.Endothelial TAGLN 1.624 4.97E−20 9.22E−01 1.52E−03 0.651 F.Endothelial TIMP1 0.703 4.10E−08 6.73E−01 7.05E−17 0.694 F.Endothelial VIM 0.938 3.36E−08 7.75E−01 2.34E−29 1.462 F.Fibroblast AREG 2.762 2.41E−20 4.30E−01 2.17E−01 0.528 F.Fibroblast C12orf75 1.837 5.90E−28 3.48E−01 1.96E−02 0.659 F.Fibroblast EMP3 0.505 1.25E−09 4.92E−01 9.97E−34 0.590 F.Fibroblast GLIPR1 1.473 3.84E−31 2.25E−01 9.47E−03 0.866 F.Fibroblast IL13RA2 5.211 6.14E−32 1.00E+00 2.254 F.Fibroblast INHBA 4.213 2.59E−21 1.00E+00 2.254 F.Fibroblast MME 4.715 1.69E−35 1.00E+00 2.254 F.Fibroblast MTRNR2L1 1.638 4.80E−70 8.33E−01 2.73E−10 1.487 F.Fibroblast PRRX1 4.491 2.38E−24 1.00E+00 2.254 F.Fibroblast PRSS23 1.544 1.03E−52 6.89E−01 9.84E−13 0.783 F.Fibroblast PTMA 0.290 8.33E−02 5.14E−01 5.87E−33 0.617 F.Fibroblast RPL7 −0.783 2.22E−06 −3.72E−01  4.41E−17 −0.992 F.Fibroblast RPS26 −0.737 2.77E−14 −3.74E−01  1.63E−16 −0.707 F.Fibroblast S100A6 0.310 7.37E−02 6.45E−01 2.95E−31 0.722 F.Fibroblast SGK1 1.600 2.79E−22 8.71E−01 2.31E−09 0.688 F.Fibroblast STC1 4.459 5.39E−24 1.00E+00 2.254 F.Fibroblast TIMP1 0.803 1.52E−10 1.07E+00  1.73E−122 0.604 F.Glia ANXA1 2.251 1.06E−07 2.05E+00 2.20E−25 4.008 F.Glia S100A3 4.450 4.92E−21 −3.87E−01  4.85E−01 0.677 F.Pcap_Venules ANXA2 0.635 1.29E−02 1.18E+00 6.99E−23 0.685 F.Pcap_Venules COL4A2 2.336 7.99E−27 5.62E−01 2.29E−04 0.910 F.Pcap_Venules FKBP1A 1.402 3.44E−04 7.98E−01 1.52E−18 0.977 F.Pcap_Venules PRKCDBP 1.778 5.49E−19 8.81E−01 2.11E−10 1.276 F.Pcap_Venules PRSS23 1.992 4.28E−22 1.13E+00 1.25E−12 1.271 F.Pcap_Venules VAMP5 2.074 1.37E−21 6.46E−01 4.93E−04 1.770 F.Stromal DEFA5 4.171 5.18E−27 1.00E+00 2.053 F.Stromal GLIPR1 1.206 3.78E−21 1.32E−01 1.41E−01 0.620 F.Stromal IL13RA2 4.847 5.21E−26 1.00E+00 2.053 F.Stromal LINC00152 0.880 1.35E−22 4.20E−01 1.13E−10 0.511 F.Stromal MME 4.368 7.34E−28 1.00E+00 2.053 F.Stromal MTRNR2L1 1.652 1.46E−93 5.61E−01 2.24E−06 1.346 F.Stromal PRRX1 4.419 1.14E−22 1.00E+00 2.053 F.Stromal RGCC 0.835 2.42E−22 2.70E−01 1.42E−02 1.006 F.Stromal RPL7 −0.662 2.11E−06 −3.05E−01  3.33E−15 −0.852 F.Stromal RPS26 −0.666 7.83E−15 −3.25E−01  1.12E−16 −0.646 F.Stromal S100A10 0.447 2.43E−09 4.83E−01 9.92E−23 0.558 F.Stromal S100A6 0.162 1.84E−01 5.76E−01 2.03E−30 0.503 F.Stromal TMSB10 0.385 2.10E−02 4.72E−01 3.46E−30 0.736 F.Villus COL3A1 1.221 2.23E−11 5.24E−01 5.11E−12 0.746 F.Villus DCN 1.537 3.42E−30 3.62E−01 1.30E−03 1.307 F.Villus IGFBP7 1.049 1.07E−03 9.90E−01 4.40E−19 1.542 F.Villus PLAC9 1.552 8.20E−31 2.20E−01 2.27E−03 0.669 F.Villus TIMP1 1.228 3.53E−08 1.21E+00 1.69E−49 1.394 F.Villus_1 DCN 2.175 1.34E−21 5.02E−01 6.38E−03 2.265 F.Villus_1 LUM 2.080 7.39E−23 5.76E−01 3.15E−02 2.117 F.Villus_1 TIMP1 1.842 1.31E−06 1.49E+00 1.35E−30 2.426 F.Villus_2 PLAC9 1.583 1.57E−19 2.01E−01 4.07E−02 0.794 F.Villus_2 TIMP1 0.864 1.72E−03 1.01E+00 2.78E−20 0.965 I.Immune AC009501.4 −0.856 2.31E−50 5.93E−02 1.52E−01 −0.784 I.Immune IGHA2 −0.760 7.42E−37 −9.80E−01  3.00E−21 −0.646 I.Lymphoid AC009501.4 −0.789 3.67E−43 3.15E−02 4.45E−01 −0.773 I.Lymphoid ANXA1 −0.548 3.52E−20 −1.52E−01  1.05E−02 −0.526 I.Lymphoid DHRS9 1.968 3.85E−20 −6.42E−02  7.68E−01 0.711 I.Lymphoid IGHA2 −0.653 8.92E−28 −7.76E−01  5.33E−13 −0.522 M.CD69pos_Mast SAMSN1 1.332 4.44E−18 3.55E−01 2.81E−06 1.064 M.CD69pos_Mast SRGN 1.688 7.65E−12 5.22E−01 1.72E−09 2.121 M.Macrophages FTL −1.951 3.23E−03 −6.58E−01  6.94E−21 −2.086 M.Mast PPAP2A 2.425 1.61E−23 1.70E−01 4.90E−01 1.631 M.Mast SAMSN1 1.258 1.50E−17 3.46E−01 9.27E−07 0.886 M.Mast SRGN 1.668 2.53E−12 5.90E−01 3.29E−13 2.145 M.Monocytes AC009501.4 −0.751 1.25E−16 2.40E−01 3.36E−05 −0.601 M.Monocytes CD300E 4.435 1.27E−19 1.00E+00 2.268 M.Monocytes CD74 −0.857 1.69E−02 −6.80E−01  5.05E−25 −0.651 M.Monocytes CST3 −0.938 4.63E−06 1.04E+00 6.47E−92 −0.611 M.Monocytes RGS1 −0.963 9.92E−27 1.23E−01 1.00E−01 −0.519 M.Myeloid CD300E 4.420 1.39E−19 1.00E+00 2.065 M.Myeloid IL2RG 0.761 5.19E−14 4.04E−01 6.77E−08 0.550 M.Myeloid JUNB −0.815 2.96E−18 −1.46E−01  9.95E−03 −0.708 M.Myeloid SH3BGRL3 0.359 2.28E−04 4.97E−01 3.22E−29 0.522 M.Myeloid TMEM176B 0.775 8.35E−22 1.47E−01 1.92E−02 0.518 M.Neutrophils CST3 −1.508 6.90E−03 −1.84E+00  4.29E−28 −1.016 M.Neutrophils TIMP1 0.622 6.08E−02 1.91E+00 6.49E−24 1.077 T.Activated_CD4_hiFos RPL39 0.601 2.66E−06 1.20E+00 1.09E−18 0.570 T.Activated_CD4_loFos ANXA1 −2.040 5.80E−37 −4.49E−01  1.65E−06 −1.270 T.Activated_CD4_loFos RPL39 0.499 1.23E−04 1.29E+00 9.00E−22 0.557 T.Activated_CD4_loFos RPS29 0.391 9.55E−02 7.71E−01 1.98E−20 0.680 T.CD4 AC009501.4 −0.674 2.50E−27 1.01E−01 3.23E−02 −0.590 T.CD4 ACP5 1.065 7.77E−22 6.83E−02 5.52E−01 0.628 T.CD4 ANXA1 −1.551  6.16E−138 −4.15E−01  4.74E−14 −0.969 T.CD4 CCL5 −1.068 1.87E−64 5.50E−02 4.40E−01 −0.675 T.CD4 CXCL13 4.921 3.71E−40 1.00E+00 1.584 T.CD4 MT-ND3 0.741 2.99E−30 6.72E−01 1.16E−16 0.679 T.CD4 NPDC1 2.292 9.11E−30 −3.40E−01  1.27E−01 0.730 T.CD4 RPL10 −0.862 3.17E−03 −3.97E−01  7.90E−40 −1.413 T.CD4 RPL13A −0.805 3.03E−03 −2.81E−01  2.44E−21 −1.161 T.CD4 RPL3 −0.487 3.75E−02 −3.65E−01  1.02E−31 −0.779 T.CD4 RPS18 −0.525 3.46E−02 −3.14E−01  1.77E−22 −0.857 T.CD4 RPS2 −0.381 1.44E−01 −3.47E−01  9.61E−25 −0.701 T.CD4 RPS3 −0.379 4.81E−02 −3.89E−01  1.29E−38 −0.531 T.CD4 RPS6 −0.737 2.86E−03 −3.12E−01  1.45E−22 −1.117 T.CD4 SRGN 0.451 3.54E−09 3.10E−01 8.66E−18 0.604 T.CD4 VIM −0.782 2.19E−38 −2.27E−01  3.69E−06 −0.853 T.CD8 ANXA1 −0.806 1.03E−25 −3.22E−01  2.67E−06 −0.760 T.CD8 CD2 0.761 8.07E−20 3.65E−01 3.50E−19 0.632 T.CD8 CD63 −0.780 2.66E−21 −3.56E−01  4.41E−11 −0.689 T.CD8 FOS −0.623 2.75E−15 −3.31E−01  1.24E−06 −0.559 T.CD8 GADD45G 1.698 2.47E−22 1.85E−01 2.17E−01 0.548 T.CD8 HLA-B 0.858 1.33E−03 4.19E−01 1.45E−22 1.265 T.CD8 RPL3 −0.622 5.58E−02 −4.10E−01  8.03E−22 −1.003 T.CD8 RPL8 −0.736 7.33E−05 −3.74E−01  2.23E−23 −0.824 T.CD8 RPS29 0.341 4.24E−03 4.98E−01 7.90E−24 0.524 T.CD8 TNFRSF4 1.540 7.08E−20 4.29E−01 2.87E−02 0.655 T.CD8 ZFP36 −0.737 4.37E−20 −2.73E−01  7.01E−07 −0.535 T.CD8_IELs KLRB1 1.674 1.58E−25 1.11E+00 1.72E−14 1.381 T.CD8_LP ANXA1 −1.174 2.14E−24 −4.29E−01  1.37E−06 −1.040 T.CD8_LP CD27 0.900 8.38E−15 4.65E−01 6.62E−10 0.522 T.CD8_LP CST7 0.910 7.31E−14 2.98E−01 3.74E−08 0.519 T.CD8_LP RPL39 0.594 1.71E−07 9.88E−01 4.26E−14 0.553 T.Cycling_T CXCR6 2.805 1.15E−19 7.05E−01 4.74E−03 1.903 T.Memory_CD4 ANXA1 −1.660 1.40E−40 −4.97E−01  2.42E−04 −1.223 T.Memory_CD4 CCL5 −1.316 1.96E−21 −2.16E−01  2.97E−01 −1.076 T.Memory_CD4 TOX2 3.301 9.76E−21 4.04E−01 3.30E−01 0.543 T.Tcells AC009501.4 −0.910 4.89E−56 4.51E−02 2.76E−01 −0.815 T.Tcells ANXA1 −0.849 1.27E−49 −1.73E−01  6.37E−04 −0.615 T.Tcells CTSH 1.589 1.59E−25 −6.19E−02  6.77E−01 0.605 T.Tcells CXCL13 4.630 3.60E−29 1.00E+00 1.874 T.Tcells NPDC1 2.424 2.51E−27 −2.81E−01  3.16E−01 0.897 T.Tcells SRGN 0.583 1.62E−16 3.28E−01 8.70E−22 0.664 T.Tcells TMSB4X −1.614 6.61E−03 −3.91E−01  8.77E−32 −2.065 T.Tcells VIM −0.618 2.92E−27 −7.84E−02  6.91E−02 −0.669 T.Tregs CD7 1.258 3.50E−22 6.20E−01 4.06E−14 1.382 T.Tregs LINC00152 1.269 6.98E−23 3.66E−01 1.55E−06 0.749 T.Tregs MIR4435-1HG 1.248 1.64E−21 3.03E−01 7.06E−05 0.533 ident pvalH n ref_n mu ref_mu total ref_total B.Bcells 1.04E−38 483 1399 2.242 2.300 0.045 0.136 B.Bcells 8.87E−74 498 432 1.766 2.020 0.148 0.154 B.Bcells 5.35E−52 450 439 2.304 1.853 0.141 0.100 B.Bcells  4.21E−189 1205 1893 4.576 3.181 0.174 0.104 B.Bcells 8.84E−89 815 780 2.462 2.103 0.215 0.160 B.Bcells 1.73E−67 412 261 2.558 2.798 0.134 0.100 B.Bcells  1.01E−110 1105 1696 3.373 2.914 0.154 0.172 B.Bcells  1.50E−111 928 1091 3.250 2.626 0.175 0.134 B.Bcells  6.18E−144 1210 1891 3.572 2.654 0.192 0.159 B.Bcells  4.50E−104 802 713 2.586 2.009 0.182 0.109 B.Bcells  5.45E−109 1197 1847 3.031 2.347 0.109 0.105 B.Bcells 1.18E−46 174 44 1.913 1.716 0.163 0.036 B.Bcells 1.38E−64 757 743 2.158 1.906 0.152 0.126 B.Bcells 8.67E−80 750 806 2.343 1.813 0.120 0.089 B.Bcells 4.24E−91 854 1210 3.282 3.224 0.225 0.306 B.Bcells  1.35E−130 820 1150 4.566 4.059 0.211 0.209 B.Bcells  2.09E−120 933 1229 3.044 2.562 0.294 0.277 B.Bcells  3.30E−125 1225 1949 4.009 2.968 0.121 0.093 B.Bcells  7.49E−158 971 1157 3.959 3.249 0.250 0.182 B.Bcells 2.57E−82 640 451 3.255 3.056 0.199 0.122 B.Bcells 7.18E−87 277 27 2.057 1.822 0.302 0.025 B.Bcells 3.70E−21 48 0 0.632 −17.176 0.031 0.000 B.Bcells 7.85E−72 470 383 2.264 2.448 0.113 0.105 B.Bcells  6.61E−145 1275 2048 4.351 3.203 0.117 0.085 B.Bcells 3.60E−38 154 39 1.755 1.769 0.148 0.038 B.Bcells 2.82E−41 155 68 1.830 0.739 0.079 0.016 B.Bcells 7.73E−62 708 864 2.165 2.088 0.173 0.200 B.Bcells 8.58E−80 1248 2005 3.488 2.912 0.109 0.118 B.Bcells 3.28E−81 865 854 2.952 2.811 0.260 0.233 B.Bcells 2.71E−63 992 1484 4.370 4.045 0.204 0.244 B.Bcells 2.64E−61 843 1074 4.756 4.445 0.214 0.220 B.Bcells 7.95E−79 779 908 4.032 3.601 0.276 0.239 B.Bcells 3.96E−47 957 1404 5.906 5.712 0.213 0.273 B.Bcells 4.69E−68 918 1220 5.136 4.581 0.230 0.208 B.Bcells 8.27E−48 204 77 2.496 2.746 0.119 0.054 B.Bcells  2.07E−180 992 2293 10.016 10.713 0.167 0.624 B.Bcells  8.01E−210 645 2002 7.927 9.053 0.111 0.750 B.Bcells  1.21E−127 911 2160 8.371 9.095 0.157 0.616 B.Bcells 9.10E−78 374 195 2.116 1.882 0.213 0.095 B.Bcells  4.00E−120 727 651 3.945 3.519 0.295 0.197 B.Bcells 2.59E−88 458 209 2.385 2.686 0.262 0.147 B.Bcells  9.96E−110 762 795 3.149 2.853 0.295 0.251 B.Bcells 1.12E−66 945 1525 2.304 1.948 0.149 0.188 B.Bcells 6.26E−26 156 73 1.943 2.469 0.087 0.059 B.Bcells 1.39E−50 631 748 4.703 4.629 0.216 0.244 B.Bcells 1.38E−44 838 1094 3.810 3.127 0.073 0.059 B.Bcells 2.52E−56 1010 1516 2.836 2.441 0.092 0.105 B.Bcells 2.40E−90 820 864 2.757 1.961 0.151 0.092 B.Bcells 8.51E−86 1095 1476 2.904 2.239 0.119 0.101 B.Bcells 1.01E−80 413 262 1.918 1.807 0.199 0.117 B.Bcells 3.65E−81 936 1235 2.460 1.948 0.163 0.151 B.Bcells 1.34E−79 484 297 2.028 2.371 0.138 0.107 B.Bcells  4.97E−138 1100 1723 3.484 2.776 0.236 0.226 B.Bcells 3.65E−95 910 1223 2.569 2.128 0.209 0.207 B.Bcells 9.44E−43 892 1968 1.978 2.456 0.060 0.183 B.Bcells 2.50E−75 1284 2234 3.998 3.235 0.115 0.118 B.Bcells 6.56E−68 1309 2259 4.110 3.482 0.110 0.123 B.Bcells 3.32E−50 380 272 2.055 1.696 0.163 0.091 B.Bcells 4.71E−50 352 269 3.503 2.736 0.235 0.106 B.Bcells 5.59E−20 85 20 1.440 2.189 0.086 0.034 B.Bcells 7.87E−80 688 594 2.676 2.613 0.241 0.199 B.Cycling 1.73E−84 247 174 7.126 5.318 0.092 0.018 B.Cycling 5.54E−43 240 144 5.178 4.016 0.073 0.020 B.Cycling 3.85E−23 209 76 2.861 2.359 0.112 0.029 B.Cycling 1.45E−42 231 133 3.844 2.892 0.070 0.021 B.Cycling 8.02E−24 212 91 3.597 3.114 0.076 0.023 B.Cycling 5.71E−47 240 151 4.273 3.328 0.093 0.030 B.Cycling 2.73E−29 229 120 3.523 2.612 0.064 0.018 B.Cycling 4.99E−23 206 61 2.958 2.422 0.088 0.018 B.Cycling 1.52E−32 190 93 3.093 2.225 0.132 0.035 B.Cycling 2.41E−49 222 99 4.402 3.454 0.135 0.031 B.Cycling 2.67E−54 249 171 5.563 4.394 0.067 0.020 B.Cycling 9.31E−40 240 162 4.498 3.578 0.140 0.050 B.Cycling 7.15E−19 206 93 3.988 3.518 0.063 0.021 B.Cycling 4.55E−24 217 86 5.384 4.656 0.071 0.017 B.Cycling 3.18E−55 244 143 4.953 3.918 0.136 0.039 B.Cycling 2.29E−26 221 94 4.563 4.045 0.293 0.087 B.Cycling 4.80E−31 235 119 3.988 3.437 0.131 0.045 B.Cycling 1.85E−61 236 128 4.838 3.643 0.207 0.049 B.Cycling 1.80E−37 238 153 4.078 3.108 0.068 0.022 B.Cycling 1.11E−34 227 117 3.716 2.806 0.081 0.022 B.Cycling 1.06E−26 216 102 2.854 1.895 0.069 0.017 B.Cycling 3.25E−26 173 53 3.612 3.180 0.109 0.025 B.Cycling 2.36E−19 140 24 2.164 1.371 0.228 0.023 B.Cycling 6.13E−21 154 31 2.328 2.730 0.136 0.036 B.Cycling 6.63E−21 220 91 3.354 2.544 0.064 0.015 B.Cycling 4.43E−23 220 115 3.195 2.347 0.073 0.021 B.Cycling 5.09E−25 188 61 2.981 2.794 0.134 0.038 B.Cycling 3.95E−23 161 31 3.630 2.981 0.363 0.045 B.Cycling 1.51E−21 187 80 2.718 2.124 0.076 0.021 B.Cycling 1.01E−23 173 85 2.356 1.536 0.148 0.041 B.Cycling 1.37E−24 238 154 4.104 3.464 0.070 0.029 B.Cycling 1.88E−33 213 91 3.527 2.469 0.090 0.018 B.Cycling 5.24E−28 201 90 2.794 2.002 0.093 0.024 B.Cycling 1.04E−27 224 114 3.694 2.991 0.110 0.034 B.Cycling 2.82E−21 187 96 4.783 3.306 0.068 0.013 B.Cycling 1.72E−20 218 84 3.978 3.890 0.237 0.086 B.Cycling 2.42E−39 238 124 4.983 4.198 0.137 0.041 B.Cycling 9.78E−42 230 99 4.397 3.556 0.175 0.042 B.FO 8.53E−24 157 191 2.338 2.889 0.082 0.146 B.FO 4.61E−29 185 172 2.828 2.996 0.103 0.108 B.FO 1.07E−42 346 886 6.547 5.472 0.077 0.093 B.FO 5.91E−33 320 636 4.777 3.888 0.067 0.071 B.FO 1.32E−19 135 153 2.756 3.301 0.060 0.099 B.FO 4.79E−20 308 663 3.749 3.828 0.071 0.162 B.FO 1.67E−19 256 441 3.575 3.342 0.077 0.113 B.FO 5.19E−21 64 22 2.335 2.708 0.086 0.038 B.FO 1.30E−19 185 216 3.051 3.392 0.120 0.178 B.FO 6.21E−22 216 330 2.583 3.130 0.086 0.191 B.FO 1.07E−37 298 736 4.974 4.587 0.122 0.231 B.FO 9.69E−29 269 464 3.294 3.481 0.140 0.274 B.FO 2.17E−21 86 46 2.090 2.916 0.068 0.064 B.FO 1.09E−39 305 593 4.035 3.817 0.113 0.189 B.FO 2.77E−23 222 293 3.507 3.312 0.104 0.120 B.FO 9.81E−33 71 3 2.270 2.417 0.112 0.005 B.FO 1.79E−18 76 28 1.912 2.337 0.106 0.052 B.FO 4.13E−26 174 198 2.430 3.137 0.057 0.106 B.FO 1.15E−19 63 17 2.007 2.685 0.081 0.035 B.FO 6.68E−31 81 15 2.190 2.182 0.062 0.011 B.FO 5.23E−28 65 6 1.842 2.346 0.148 0.019 B.FO 8.78E−20 199 311 2.591 2.886 0.058 0.112 B.FO 1.78E−40 209 240 2.609 2.695 0.101 0.124 B.FO 3.07E−20 158 202 2.279 2.676 0.104 0.175 B.FO 8.54E−19 109 105 2.143 2.803 0.031 0.047 B.FO 1.04E−22 347 882 5.567 5.194 0.053 0.104 B.FO 1.31E−28 81 34 2.751 2.799 0.066 0.029 B.FO 2.61E−22 135 655 8.300 7.716 0.080 0.258 B.FO 1.06E−19 165 171 2.806 2.748 0.078 0.078 B.FO 5.92E−39 140 70 2.395 2.901 0.121 0.086 B.FO 2.11E−40 278 466 4.067 3.725 0.161 0.213 B.FO 6.19E−25 139 115 2.181 2.949 0.097 0.137 B.FO 4.78E−30 249 388 3.235 3.400 0.145 0.254 B.FO 1.00E−20 251 426 2.947 3.109 0.083 0.157 B.FO 6.31E−20 149 153 2.368 3.076 0.047 0.079 B.FO 1.65E−28 139 97 1.987 2.737 0.099 0.116 B.FO 1.57E−30 166 157 2.351 2.981 0.072 0.105 B.FO 6.28E−37 301 615 4.006 3.826 0.125 0.226 B.FO 2.83E−22 249 406 2.957 3.220 0.098 0.192 B.FO 2.31E−21 205 336 3.024 3.304 0.142 0.283 B.FO 1.36E−19 131 137 3.426 2.895 0.069 0.050 B.FO 4.87E−26 157 137 2.445 2.712 0.124 0.131 B.FO 1.32E−24 107 60 2.219 2.971 0.061 0.058 B.FO 1.17E−20 109 72 1.997 2.474 0.043 0.040 B.GC 3.38E−20 184 94 7.326 6.520 0.079 0.023 B.GC 1.04E−20 176 62 4.966 4.158 0.107 0.021 B.GC 1.14E−19 168 48 4.267 3.147 0.187 0.025 B.Plasma 1.27E−28 72 11 1.428 −0.956 0.061 0.002 B.Plasma  2.63E−150 513 1325 10.681 11.221 0.162 0.606 B.Plasma  5.56E−177 443 1319 8.371 9.410 0.118 0.720 B.Plasma  1.78E−118 509 1326 8.796 9.476 0.144 0.601 B.Plasma 5.02E−20 47 10 3.860 0.076 0.161 0.002 B.Plasma 2.94E−25 349 1113 2.132 2.616 0.056 0.252 B.Plasma 1.44E−24 430 1235 1.500 1.718 0.025 0.083 E.Absorptive 3.63E−67 96 1244 3.047 2.477 0.017 0.146 E.Absorptive 2.65E−21 368 1671 7.505 7.222 0.048 0.179 E.Absorptive 1.21E−42 190 387 1.659 1.214 0.063 0.094 E.Absorptive 5.55E−32 88 17 −0.143 0.976 0.035 0.015 E.Absorptive 1.59E−43 258 628 1.227 0.982 0.034 0.071 E.Absorptive 2.53E−33 305 1551 3.289 4.431 0.035 0.393 E.Absorptive 3.05E−49 98 14 4.137 1.495 0.224 0.005 E.Absorptive 1.67E−21 65 25 0.004 0.987 0.017 0.013 E.Absorptive 1.41E−19 39 4 0.106 0.014 0.024 0.002 E.Absorptive 6.06E−21 53 21 0.786 0.777 0.060 0.023 E.Absorptive 1.28E−32 339 1314 3.011 2.752 0.057 0.184 E.Absorptive 9.74E−40 368 1639 5.426 4.978 0.048 0.156 E.Absorptive 5.58E−67 294 498 2.895 1.921 0.029 0.025 E.Absorptive 1.89E−28 336 1328 2.345 2.218 0.035 0.127 E.Absorptive 3.06E−35 251 1384 2.155 3.528 0.019 0.264 E.Absorptive 4.77E−33 54 0 2.628 −16.350 0.305 0.000 E.Absorptive 1.89E−20 74 87 2.443 1.702 0.089 0.062 E.Absorptive 2.35E−43 219 378 2.533 1.516 0.027 0.023 E.Absorptive 9.93E−59 265 638 1.643 1.188 0.053 0.093 E.Absorptive 4.23E−45 344 1349 2.750 2.245 0.034 0.093 E.Absorptive 5.24E−40 291 857 1.725 1.341 0.034 0.077 E.Absorptive 1.68E−19 367 1664 5.041 5.531 0.048 0.303 E.Absorptive 7.19E−24 60 7 −0.129 0.206 0.061 0.009 E.Absorptive 1.86E−24 54 0 4.033 −16.350 0.787 0.000 E.Absorptive  2.07E−114 348 1120 3.784 2.433 0.184 0.233 E.Absorptive 1.59E−26 53 2 −0.482 2.042 0.038 0.008 E.Absorptive 1.33E−24 69 44 0.194 0.781 0.030 0.029 E.Absorptive 8.20E−35 95 29 0.344 0.063 0.098 0.025 E.Absorptive 6.88E−20 85 89 0.778 0.921 0.042 0.049 E.Absorptive 1.36E−64 245 306 3.534 1.581 0.107 0.035 E.Absorptive 3.60E−32 198 380 0.437 0.549 0.017 0.035 E.Absorptive 2.80E−49 281 838 1.844 1.287 0.044 0.089 E.Absorptive 1.14E−50 346 1269 2.922 2.023 0.059 0.117 E.Absorptive 1.05E−83 298 675 2.781 2.124 0.100 0.144 E.Absorptive 7.50E−46 100 21 3.802 0.828 0.058 0.002 E.Absorptive 2.22E−68 249 318 2.422 1.037 0.071 0.035 E.Absorptive 3.20E−94 259 597 3.764 1.869 0.067 0.042 E.Absorptive 1.62E−20 371 1672 7.159 6.231 0.106 0.252 E.Absorptive 6.48E−38 78 3 2.437 0.683 0.116 0.001 E.Absorptive 2.00E−35 298 1066 4.479 3.742 0.111 0.238 E.Absorptive 1.02E−28 283 1390 2.314 2.850 0.018 0.131 E.Absorptive 8.49E−41 89 0 1.292 16.350 0.525 0.000 E.Absorptive 3.41E−37 90 123 1.233 0.242 0.030 0.021 E.Absorptive 3.92E−50 164 116 2.724 1.038 0.080 0.018 E.Absorptive 6.82E−77 282 511 3.886 2.445 0.134 0.089 E.Absorptive 6.35E−35 148 205 1.012 0.544 0.029 0.029 E.Absorptive 1.58E−23 40 0 0.468 −16.350 0.127 0.000 E.Absorptive 3.03E−25 94 68 1.088 0.087 0.045 0.016 E.Absorptive_All  5.06E−183 499 1770 3.543 2.771 0.096 0.200 E.Absorptive_All  1.07E−103 1420 1658 4.318 3.137 0.192 0.099 E.Absorptive_All 1.07E−28 369 140 1.080 1.047 0.042 0.016 E.Absorptive_All 2.98E−40 196 11 0.329 0.516 0.083 0.005 E.Absorptive_All 8.56E−75 1546 2357 4.293 4.737 0.122 0.254 E.Absorptive_All 2.66E−88 344 23 3.817 1.783 0.413 0.007 E.Absorptive_All 6.90E−30 119 3 0.444 −0.040 0.170 0.003 E.Absorptive_All 3.80E−71 1056 1138 2.072 1.589 0.084 0.065 E.Absorptive_All 3.95E−77 1522 2444 7.166 7.331 0.214 0.385 E.Absorptive_All 9.02E−37 856 1500 2.216 2.345 0.032 0.062 E.Absorptive_All 2.50E−26 105 5 0.881 0.092 0.090 0.002 E.Absorptive_All 3.01E−23 1735 2489 7.437 7.860 0.150 0.289 E.Absorptive_All 1.08E−71 1624 2409 4.913 5.477 0.066 0.146 E.Absorptive_All 3.03E−23 91 0 0.408 −17.539 0.638 0.000 E.Absorptive_All 4.82E−35 1419 1960 3.283 2.913 0.073 0.078 E.Absorptive_All 3.80E−54 431 141 1.562 1.256 0.089 0.024 E.Absorptive_All 3.16E−22 160 36 0.933 1.601 0.042 0.015 E.Absorptive_All  3.42E−125 920 460 3.002 1.778 0.087 0.019 E.Absorptive_All 7.80E−22 69 0 2.368 −17.539 0.257 0.000 E.Absorptive_All 6.50E−31 177 17 0.337 1.431 0.037 0.007 E.Absorptive_All 3.04E−73 773 591 2.612 1.755 0.084 0.036 E.Absorptive_All 7.60E−77 730 452 1.506 1.165 0.108 0.053 E.Absorptive_All 1.54E−46 843 1549 1.949 2.368 0.041 0.100 E.Absorptive_All 1.46E−21 76 0 0.542 −17.539 0.169 0.000 E.Absorptive_All 3.29E−38 325 84 2.983 1.893 0.082 0.010 E.Absorptive_All 1.64E−23 93 0 3.614 −17.539 0.846 0.000 E.Absorptive_All 1.12E−51 620 634 5.729 4.769 0.196 0.103 E.Absorptive_All 7.61E−35 1588 2402 4.612 4.908 0.127 0.236 E.Absorptive_All  1.04E−116 729 219 3.864 2.852 0.385 0.057 E.Absorptive_All 1.04E−39 159 2 0.058 1.779 0.118 0.005 E.Absorptive_All 3.45E−56 1691 2487 7.162 7.586 0.193 0.381 E.Absorptive_All  2.14E−274 1177 517 4.189 2.265 0.436 0.050 E.Absorptive_All 1.39E−28 1505 2317 4.054 4.443 0.135 0.272 E.Absorptive_All 1.83E−85 739 442 2.499 2.072 0.170 0.076 E.Absorptive_All 3.67E−46 155 3 2.961 1.219 0.259 0.002 E.Absorptive_All  1.17E−117 432 39 4.135 1.191 0.214 0.003 E.Absorptive_All  3.25E−102 833 482 2.349 1.403 0.161 0.048 E.Absorptive_All  2.68E−202 1159 957 3.596 2.147 0.197 0.060 E.Absorptive_All 1.74E−95 1745 2469 6.831 5.829 0.275 0.194 E.Absorptive_All 2.81E−65 259 3 2.452 1.956 0.265 0.002 E.Absorptive_All 0.00E+00 1060 152 3.259 1.072 0.406 0.013 E.Absorptive_All 1.13E−53 983 971 4.085 3.343 0.238 0.140 E.Absorptive_All 5.91E−55 1159 1974 2.878 3.300 0.078 0.177 E.Absorptive_All 3.95E−49 216 0 1.169 −17.539 0.707 0.000 E.Absorptive_All 9.70E−52 255 89 1.308 0.390 0.076 0.014 E.Absorptive_All 2.95E−67 465 106 2.102 1.260 0.117 0.015 E.Absorptive_All  6.51E−168 910 319 3.398 2.057 0.183 0.025 E.Absorptive_All  3.72E−205 683 37 2.154 0.887 0.059 0.001 E.Absorptive_All 4.74E−59 213 2 2.231 0.680 0.657 0.002 E.Absorptive_All 1.02E−25 109 6 0.210 0.649 0.066 0.005 E.Absorptive_All 8.34E−31 325 165 0.971 0.712 0.056 0.024 E.Absorptive_All 9.55E−19 63 0 0.619 −17.539 0.153 0.000 E.Absorptive_All 4.63E−21 82 0 −0.334 −17.539 0.382 0.000 E.Absorptive_TA_1 6.59E−22 287 1127 4.349 4.683 0.038 0.188 E.Absorptive_TA_1 9.35E−22 32 0 2.997 −16.123 0.159 0.000 E.Absorptive_TA_1 1.86E−32 48 0 4.117 −16.123 0.280 0.000 E.Absorptive_TA_1 2.17E−20 282 1113 4.277 4.599 0.032 0.156 E.Absorptive_TA_1 3.94E−33 305 1175 4.861 5.329 0.041 0.218 E.Absorptive_TA_1 5.38E−23 124 181 6.262 5.640 0.098 0.093 E.Absorptive_TA_1 4.01E−53 158 124 3.474 2.132 0.107 0.033 E.Absorptive_TA_1 2.90E−52 113 28 4.725 2.681 0.184 0.011 E.Absorptive_TA_1 1.29E−49 89 10 5.391 2.272 0.137 0.002 E.Absorptive_TA_1 1.17E−23 345 1190 5.632 6.131 0.028 0.139 E.Absorptive_TA_1 5.40E−24 288 1114 4.851 5.283 0.024 0.127 E.Absorptive_TA_1 1.45E−18 324 1160 4.973 5.378 0.034 0.159 E.Absorptive_TA_1 7.17E−23 284 1135 4.886 5.183 0.038 0.186 E.Absorptive_TA_1 1.97E−25 326 1166 5.373 5.832 0.030 0.146 E.Absorptive_TA_1 1.05E−19 353 1201 6.053 6.492 0.036 0.167 E.Absorptive_TA_1 2.64E−24 342 1178 5.895 6.451 0.032 0.162 E.Absorptive_TA_1 1.39E−20 248 1066 4.626 4.803 0.030 0.147 E.Absorptive_TA_1 2.31E−26 200 420 4.010 2.805 0.061 0.056 E.Absorptive_TA_1 2.27E−63 118 16 3.177 2.420 0.090 0.007 E.Absorptive_TA_1 1.88E−19 28 0 4.104 −16.123 0.206 0.000 E.Absorptive_TA_2 1.67E−49 108 978 2.753 2.209 0.016 0.099 E.Absorptive_TA_2 5.72E−26 244 762 1.317 1.042 0.018 0.046 E.Absorptive_TA_2 2.03E−32 230 709 1.100 0.888 0.020 0.052 E.Absorptive_TA_2 1.04E−29 125 136 0.487 0.004 0.017 0.014 E.Absorptive_TA_2 3.17E−27 80 33 3.099 1.067 0.101 0.010 E.Absorptive_TA_2 3.39E−26 0 196 15.775 1.382 0.000 0.414 E.Absorptive_TA_2 9.60E−35 179 1000 1.859 2.173 0.006 0.045 E.Absorptive_TA_2 9.89E−63 285 1071 3.715 2.380 0.129 0.192 E.Absorptive_TA_2 3.17E−36 236 723 2.088 1.210 0.021 0.035 E.Absorptive_TA_2 1.48E−30 174 955 1.427 1.858 0.007 0.054 E.Absorptive_TA_2 6.59E−27 286 1098 4.565 3.788 0.069 0.155 E.Absorptive_TA_2 1.08E−21 284 1168 5.498 6.173 0.051 0.335 E.Absorptive_TA_2  8.69E−134 260 393 2.514 0.418 0.092 0.033 E.Absorptive_TA_2 4.16E−65 203 174 3.529 2.182 0.143 0.048 E.Absorptive_TA_2 6.47E−27 52 0 −0.858 −15.775 0.028 0.000 E.Absorptive_TA_2 4.48E−63 258 869 2.012 1.269 0.042 0.084 E.Absorptive_TA_2 4.35E−74 181 98 4.252 1.520 0.207 0.017 E.Absorptive_TA_2 2.15E−36 0 223 −15.775 0.428 0.000 0.383 E.Absorptive_TA_2  5.99E−156 275 640 4.217 1.691 0.176 0.071 E.Absorptive_TA_2  3.72E−119 263 173 2.341 1.663 0.191 0.079 E.Absorptive_TA_2 2.16E−31 194 453 1.214 0.782 0.022 0.037 E.Absorptive_TA_2 5.48E−24 278 1099 2.848 2.347 0.047 0.130 E.Absorptive_TA_2 1.17E−62 133 38 2.935 0.315 0.044 0.002 E.Absorptive_TA_2 8.97E−33 217 469 1.352 0.707 0.033 0.046 E.Absorptive_TA_2 1.52E−35 0 128 −15.775 0.241 0.000 0.480 E.Absorptive_TA_2 4.75E−20 277 1164 3.804 3.300 0.032 0.096 E.Absorptive_TA_2 8.98E−21 287 1160 4.829 4.037 0.064 0.149 E.Absorptive_TA_2 9.43E−84 282 1031 3.086 1.900 0.045 0.073 E.Absorptive_TA_2 1.75E−23 288 1168 6.355 5.263 0.063 0.120 E.Absorptive_TA_2 3.59E−28 67 3 1.502 1.961 0.049 0.003 E.Absorptive_TA_2  3.81E−179 264 91 2.802 0.469 0.146 0.010 E.Absorptive_TA_2 4.03E−27 162 295 0.156 0.557 0.014 0.033 E.Absorptive_TA_2 7.64E−24 276 1102 3.102 2.616 0.024 0.068 E.Absorptive_TA_2 2.21E−42 157 126 0.848 0.179 0.021 0.010 E.Absorptive_TA_2 5.98E−24 280 1075 2.697 2.218 0.031 0.085 E.Absorptive_TA_2 1.80E−23 79 19 −0.213 −0.276 0.035 0.008 E.Absorptive_TA_2 1.86E−55 168 76 0.440 0.306 0.071 0.029 E.Best4_Enterocytes 2.05E−22 25 560 2.688 2.214 0.004 0.061 E.Best4_Enterocytes 1.82E−27 26 382 3.039 4.311 0.004 0.148 E.Best4_Enterocytes 2.45E−22 96 270 1.260 0.959 0.018 0.041 E.Best4_Enterocytes 7.78E−29 101 353 1.532 1.073 0.026 0.065 E.Best4_Enterocytes 9.26E−22 115 620 2.667 2.338 0.012 0.050 E.Best4_Enterocytes 1.81E−21 105 447 1.823 1.591 0.014 0.049 E.Best4_Enterocytes 3.05E−31 107 429 2.315 1.465 0.039 0.088 E.Best4_Enterocytes 6.68E−26 110 369 2.730 2.114 0.045 0.099 E.Best4_Enterocytes 2.87E−19 114 679 4.122 3.100 0.021 0.063 E.Best4_Enterocytes 1.99E−19 114 667 3.374 2.549 0.019 0.064 E.Best4_Enterocytes 7.59E−39 99 459 4.832 2.087 0.035 0.024 E.Best4_Enterocytes 2.80E−32 111 503 3.229 2.037 0.021 0.042 E.Cycling_TA 5.07E−54 192 73 −0.165 −0.156 0.064 0.024 E.Cycling_TA 3.68E−32 229 414 0.233 0.023 0.016 0.025 E.Cycling_TA 1.26E−65 295 772 1.373 0.610 0.023 0.036 E.Cycling_TA 7.50E−29 99 20 −0.848 −0.545 0.023 0.006 E.Cycling_TA 3.57E−43 290 712 0.945 0.435 0.038 0.066 E.Cycling_TA 2.72E−21 43 0 0.046 −16.039 0.400 0.000 E.Cycling_TA 3.31E−41 300 884 1.345 0.986 0.019 0.043 E.Cycling_TA 2.46E−45 95 1 1.899 −0.996 0.129 0.000 E.Cycling_TA 8.52E−60 335 1115 3.118 2.367 0.070 0.138 E.Cycling_TA 2.85E−25 0 196 −16.039 1.191 0.000 0.437 E.Cycling_TA 2.76E−29 86 4 0.594 −0.174 0.046 0.001 E.Cycling_TA 1.58E−26 331 1124 3.177 2.784 0.020 0.051 E.Cycling_TA 3.05E−44 185 168 0.709 −0.238 0.027 0.013 E.Cycling_TA 1.83E−63 216 187 2.645 0.621 0.020 0.004 E.Cycling_TA 2.09E−63 300 721 1.352 0.729 0.034 0.053 E.Cycling_TA 2.00E−24 109 52 −0.617 0.124 0.014 0.012 E.Cycling_TA 8.80E−54 313 920 1.986 0.980 0.026 0.038 E.Cycling_TA 2.28E−19 261 1008 1.140 1.931 0.009 0.062 E.Cycling_TA 2.25E−57 317 1010 2.274 1.402 0.041 0.072 E.Cycling_TA 9.20E−24 150 106 1.316 0.861 0.015 0.008 E.Cycling_TA 2.07E−20 59 0 1.276 −16.039 0.363 0.000 E.Cycling_TA 2.71E−22 171 276 3.852 3.351 0.032 0.037 E.Cycling_TA  8.20E−110 312 552 1.899 0.016 0.077 0.037 E.Cycling_TA 1.01E−89 317 963 1.906 1.041 0.047 0.078 E.Cycling_TA 3.95E−49 166 87 3.890 0.168 0.152 0.006 E.Cycling_TA 4.80E−33 77 6 −0.386 −0.939 0.027 0.001 E.Cycling_TA 3.04E−38 0 215 −16.039 0.091 0.000 0.312 E.Cycling_TA  8.54E−128 327 766 3.655 1.479 0.155 0.080 E.Cycling_TA  4.47E−117 317 204 2.128 1.458 0.193 0.078 E.Cycling_TA 1.15E−67 284 737 1.509 0.823 0.037 0.059 E.Cycling_TA 8.16E−64 332 1109 3.154 2.406 0.065 0.130 E.Cycling_TA  1.65E−110 218 71 3.325 −0.106 0.088 0.003 E.Cycling_TA 1.40E−42 330 1123 3.010 2.584 0.036 0.091 E.Cycling_TA 3.72E−25 326 1148 3.522 3.094 0.052 0.137 E.Cycling_TA 4.98E−19 338 1144 4.344 3.572 0.057 0.113 E.Cycling_TA  2.88E−110 330 1020 2.905 1.523 0.049 0.058 E.Cycling_TA  3.37E−161 300 75 1.995 −0.225 0.102 0.005 E.Cycling_TA 3.06E−38 88 0 1.949 −16.039 0.160 0.000 E.Cycling_TA 3.67E−41 329 1104 3.205 2.516 0.031 0.064 E.Cycling_TA 2.07E−50 322 1015 1.589 1.204 0.039 0.094 E.Cycling_TA 1.10E−44 175 44 −0.361 −0.773 0.046 0.009 E.Cycling_TA 3.35E−30 70 2 0.257 −1.101 0.074 0.001 E.Cycling_TA 1.82E−45 327 1094 2.266 1.793 0.044 0.107 E.Enterocyte_Immature_1 3.94E−30 71 674 3.489 2.577 0.018 0.091 E.Enterocyte_Immature_1 1.62E−39 76 50 3.467 1.480 0.127 0.021 E.Enterocyte_Immature_1 1.14E−34 59 29 2.781 1.184 0.113 0.018 E.Enterocyte_Immature_1 6.80E−19 194 876 3.054 3.556 0.017 0.111 E.Enterocyte_Immature_1 1.66E−56 104 36 3.813 1.624 0.065 0.005 E.Enterocyte_Immature_1 1.71E−23 99 143 3.221 2.143 0.053 0.036 E.Enterocyte_Immature_1 3.70E−52 80 13 3.021 1.017 0.060 0.002 E.Enterocyte_Immature_1 1.08E−18 24 0 3.099 −15.690 0.276 0.000 E.Enterocyte_Immature_1 1.45E−20 65 94 3.071 1.521 0.090 0.044 E.Enterocyte_Immature_2 1.28E−73 65 980 3.494 2.688 0.015 0.133 E.Enterocyte_Immature_2 1.33E−57 237 900 3.860 1.992 0.043 0.045 E.Enterocyte_Immature_2 9.38E−60 112 983 3.543 4.692 0.018 0.354 E.Enterocyte_Immature_2 1.01E−30 79 40 0.025 0.252 0.027 0.016 E.Enterocyte_Immature_2 2.72E−30 60 11 3.704 1.756 0.171 0.008 E.Enterocyte_Immature_2 3.06E−48 246 967 3.873 2.885 0.115 0.228 E.Enterocyte_Immature_2 5.41E−68 189 301 1.953 0.832 0.140 0.102 E.Enterocyte_Immature_2 1.07E−22 57 24 1.056 0.286 0.074 0.018 E.Enterocyte_Immature_2 5.95E−34 173 431 1.181 0.348 0.032 0.045 E.Enterocyte_Immature_2 2.38E−39 78 4 0.534 −0.290 0.088 0.003 E.Enterocyte_Immature_2 1.08E−36 64 9 3.656 0.681 0.116 0.002 E.Enterocyte_Immature_2 1.07E−22 52 15 1.809 0.622 0.050 0.006 E.Enterocyte_Immature_2 5.04E−24 199 756 1.317 0.913 0.012 0.035 E.Enterocyte_Immature_2 1.14E−34 120 99 0.559 0.331 0.038 0.027 E.Enterocyte_Immature_2 4.30E−40 88 736 0.584 1.254 0.005 0.069 E.Enterocyte_Immature_2 9.39E−26 249 1141 5.004 5.844 0.014 0.113 E.Enterocyte_Immature_2 6.11E−73 196 528 3.327 1.076 0.088 0.050 E.Enterocyte_Immature_2 1.54E−49 166 470 1.710 0.659 0.025 0.034 E.Enterocyte_Immature_2 4.27E−24 230 1103 2.452 3.667 0.022 0.243 E.Enterocyte_Immature_2 1.05E−37 169 330 0.959 0.556 0.024 0.035 E.Enterocyte_Immature_2 6.48E−20 144 288 1.805 1.058 0.044 0.052 E.Enterocyte_Immature_2  4.08E−124 239 796 3.756 1.942 0.168 0.159 E.Enterocyte_Immature_2 6.48E−37 199 703 1.494 0.811 0.024 0.052 E.Enterocyte_Immature_2 9.63E−37 0 266 −15.642 0.429 0.000 0.428 E.Enterocyte_Immature_2  6.71E−124 213 202 3.893 1.041 0.130 0.017 E.Enterocyte_Immature_2 8.08E−42 141 237 1.227 0.480 0.021 0.021 E.Enterocyte_Immature_2 3.46E−36 166 294 1.462 0.586 0.029 0.028 E.Enterocyte_Immature_2  2.39E−115 216 455 3.102 0.909 0.039 0.018 E.Enterocyte_Immature_2 1.71E−32 253 1145 7.420 6.162 0.101 0.190 E.Enterocyte_Immature_2 1.09E−35 60 0 2.563 −15.642 0.112 0.000 E.Enterocyte_Immature_2  7.40E−209 229 130 3.547 0.233 0.202 0.012 E.Enterocyte_Immature_2 2.47E−25 43 0 0.839 −15.642 0.034 0.000 E.Enterocyte_Immature_2 9.10E−37 152 319 0.941 0.464 0.021 0.031 E.Enterocyte_Immature_2 6.64E−21 47 2 −0.567 −0.713 0.036 0.001 E.Enterocyte_Immature_2 4.54E−38 225 691 3.275 2.417 0.053 0.089 E.Enterocyte_Immature_2 2.54E−29 55 0 −0.463 −15.642 0.043 0.000 E.Enterocyte_Immature_2 1.75E−25 53 0 0.218 −15.642 0.229 0.000 E.Enterocyte_Immature_2 1.94E−81 191 166 2.581 0.688 0.048 0.011 E.Enterocyte_Immature_2 1.39E−18 50 30 0.011 −0.183 0.022 0.012 E.Enterocyte_Immature_2 2.93E−32 54 0 1.504 −15.642 0.221 0.000 E.Enterocyte_Immature_2 6.20E−34 184 486 1.050 0.498 0.031 0.056 E.Enterocyte_Immature_2 1.12E−27 114 164 0.468 0.336 0.019 0.026 E.Enterocyte_Progenitor 6.40E−33 43 730 4.134 2.797 0.016 0.109 E.Enterocyte_Progenitor 1.04E−19 154 718 4.526 3.249 0.040 0.078 E.Enterocyte_Progenitor 1.54E−24 36 8 3.640 3.171 0.109 0.017 E.Enterocyte_Progenitor 9.54E−33 125 399 3.877 2.457 0.074 0.088 E.Enterocyte_Progenitor 9.52E−28 51 45 3.397 1.546 0.113 0.028 E.Enterocyte_Progenitor 2.55E−26 36 6 4.054 2.459 0.076 0.004 E.Enterocyte_Progenitor 5.02E−24 38 20 3.835 1.636 0.091 0.010 E.Enterocyte_Progenitor 6.59E−34 37 0 3.588 −15.791 0.160 0.000 E.Enterocyte_Progenitor 2.31E−40 126 372 3.980 2.527 0.083 0.089 E.Enterocyte_Progenitor 4.70E−28 88 985 3.157 3.622 0.014 0.219 E.Enterocyte_Progenitor 1.65E−63 101 124 5.392 2.337 0.175 0.026 E.Enterocyte_Progenitor 1.61E−36 58 25 3.823 2.042 0.063 0.008 E.Enterocyte_Progenitor 4.98E−59 96 108 5.484 2.505 0.251 0.036 E.Enterocyte_Progenitor 8.16E−74 122 118 4.703 2.794 0.123 0.032 E.Enterocyte_Progenitor 1.20E−42 125 359 4.224 2.418 0.047 0.039 E.Enterocyte_Progenitor 3.89E−26 205 1181 7.046 5.789 0.067 0.161 E.Enterocyte_Progenitor 1.22E−24 27 0 3.071 −15.791 0.059 0.000 E.Enterocyte_Progenitor  6.78E−108 128 33 3.785 1.938 0.141 0.010 E.Enterocyte_Progenitor 7.32E−28 56 40 3.942 1.617 0.030 0.004 E.Enterocyte_Progenitor 2.35E−19 21 0 2.816 −15.791 0.224 0.000 E.Enterocyte_Progenitor 9.85E−21 162 974 4.744 3.701 0.022 0.064 E.Enterocytes 3.29E−54 71 684 3.154 2.661 0.014 0.097 E.Enterocytes 1.87E−38 112 57 0.696 0.222 0.053 0.019 E.Enterocytes 3.02E−42 175 293 1.501 0.733 0.030 0.029 E.Enterocytes 6.23E−42 218 834 3.330 4.681 0.032 0.317 E.Enterocytes 1.14E−38 97 99 1.409 0.445 0.024 0.012 E.Enterocytes 3.73E−44 100 43 1.540 0.413 0.045 0.009 E.Enterocytes 5.35E−22 0 94 15.546 0.155 0.000 0.226 E.Enterocytes 1.50E−52 127 109 2.084 0.480 0.093 0.026 E.Enterocytes 6.97E−43 97 7 1.678 −0.684 0.234 0.003 E.Enterocytes 3.97E−44 87 9 4.272 1.896 0.211 0.004 E.Enterocytes 3.20E−37 92 32 3.499 1.773 0.173 0.018 E.Enterocytes 4.28E−21 36 0 0.182 −15.546 0.021 0.000 E.Enterocytes 8.51E−32 248 841 8.636 9.465 0.060 0.359 E.Enterocytes 1.07E−29 65 0 0.184 −15.546 0.301 0.000 E.Enterocytes 4.72E−24 88 51 1.237 0.074 0.021 0.006 E.Enterocytes 4.32E−56 126 118 3.658 0.425 0.078 0.008 E.Enterocytes 3.48E−31 178 762 1.690 2.598 0.018 0.147 E.Enterocytes 1.36E−39 209 841 6.294 6.837 0.080 0.466 E.Enterocytes 4.28E−22 248 839 5.747 5.340 0.044 0.111 E.Enterocytes 1.24E−34 192 391 1.815 1.378 0.071 0.107 E.Enterocytes 2.75E−27 49 0 2.465 −15.546 0.268 0.000 E.Enterocytes 1.91E−46 136 88 2.979 1.572 0.022 0.005 E.Enterocytes 5.18E−37 194 479 1.779 1.105 0.047 0.073 E.Enterocytes 5.39E−27 229 729 2.790 2.162 0.024 0.049 E.Enterocytes 1.93E−19 51 4 −0.021 −0.302 0.043 0.003 E.Enterocytes 3.42E−27 186 410 1.667 1.006 0.022 0.030 E.Enterocytes 4.00E−22 53 4 −0.068 0.548 0.061 0.007 E.Enterocytes 4.33E−31 192 303 1.701 1.062 0.038 0.039 E.Enterocytes 5.17E−23 50 0 4.122 −15.546 0.762 0.000 E.Enterocytes 3.74E−52 131 100 2.405 0.805 0.115 0.029 E.Enterocytes 8.63E−29 91 26 2.903 0.208 0.055 0.002 E.Enterocytes 6.89E−36 77 9 0.446 −0.229 0.082 0.006 E.Enterocytes 2.67E−47 0 244 −15.546 0.626 0.000 0.468 E.Enterocytes 3.02E−64 171 320 2.578 0.513 0.039 0.018 E.Enterocytes 3.85E−22 73 44 0.926 0.707 0.042 0.022 E.Enterocytes 1.04E−77 165 60 3.837 0.490 0.099 0.004 E.Enterocytes 1.03E−22 125 204 0.722 0.347 0.013 0.016 E.Enterocytes 3.27E−44 189 499 2.170 1.288 0.040 0.058 E.Enterocytes 3.47E−57 233 675 3.182 1.867 0.054 0.063 E.Enterocytes 7.65E−68 235 528 3.016 2.234 0.096 0.125 E.Enterocytes 4.84E−37 73 7 4.233 1.021 0.059 0.001 E.Enterocytes 2.15E−53 173 165 2.644 1.062 0.061 0.019 E.Enterocytes 9.71E−97 148 94 4.066 0.314 0.051 0.002 E.Enterocytes 1.77E−36 68 0 2.542 −15.546 0.102 0.000 E.Enterocytes 4.50E−63 139 41 3.038 0.623 0.104 0.006 E.Enterocytes 2.34E−28 58 0 0.669 −15.546 0.088 0.000 E.Enterocytes 2.33E−32 72 0 1.442 −15.546 0.466 0.000 E.Enterocytes 4.92E−34 76 86 1.177 0.259 0.027 0.016 E.Enterocytes 5.42E−25 241 837 4.131 4.960 0.057 0.350 E.Enterocytes 7.96E−26 77 13 0.155 1.455 0.041 0.017 E.Enterocytes 3.08E−59 203 332 4.155 2.209 0.138 0.059 E.Enterocytes 3.29E−38 75 1 2.458 0.451 0.473 0.002 E.Enterocytes 1.62E−23 103 83 0.758 0.933 0.025 0.022 E.Enterocytes 1.71E−28 125 147 1.130 0.424 0.025 0.018 E.Enterocytes 1.80E−21 63 24 1.327 0.022 0.037 0.006 E.Epithelial  2.13E−159 839 1715 3.231 2.717 0.119 0.170 E.Epithelial 6.16E−24 198 35 3.025 2.847 0.024 0.004 E.Epithelial 4.46E−35 338 14 0.143 0.148 0.115 0.005 E.Epithelial 6.55E−22 98 0 0.913 −17.770 0.806 0.000 E.Epithelial 1.02E−19 199 26 0.696 0.389 0.079 0.008 E.Epithelial 4.64E−24 247 26 0.592 0.061 0.034 0.002 E.Epithelial 3.31E−70 497 46 3.316 1.590 0.418 0.012 E.Epithelial 1.08E−43 424 747 1.433 1.137 0.009 0.012 E.Epithelial 2.34E−21 165 1 0.116 −0.004 0.175 0.001 E.Epithelial 5.29E−66 1547 1170 1.943 1.519 0.088 0.050 E.Epithelial 4.84E−31 893 1001 1.392 1.587 0.028 0.036 E.Epithelial 4.88E−24 231 4 −0.302 1.057 0.061 0.003 E.Epithelial 4.23E−24 226 5 1.148 −0.241 0.131 0.001 E.Epithelial 6.77E−34 1353 1568 2.315 2.483 0.045 0.059 E.Epithelial 2.80E−74 2283 2393 4.849 5.360 0.080 0.119 E.Epithelial 1.44E−24 227 38 1.658 2.925 0.060 0.024 E.Epithelial 2.14E−47 1986 2179 4.030 4.341 0.119 0.162 E.Epithelial 1.92E−58 692 142 1.358 1.060 0.093 0.016 E.Epithelial 2.37E−21 308 33 0.569 1.572 0.047 0.010 E.Epithelial 9.94E−27 448 147 1.699 1.108 0.054 0.012 E.Epithelial 1.41E−50 1618 1351 2.237 2.072 0.100 0.074 E.Epithelial 7.08E−25 178 0 −0.162 −17.770 0.545 0.000 E.Epithelial 3.12E−19 323 39 0.084 0.665 0.039 0.007 E.Epithelial 3.67E−20 524 197 1.037 1.273 0.024 0.010 E.Epithelial 5.76E−72 933 330 1.322 1.311 0.091 0.032 E.Epithelial 1.40E−55 1348 1663 2.104 2.505 0.063 0.102 E.Epithelial 9.47E−68 633 107 2.974 2.402 0.126 0.014 E.Epithelial 5.73E−32 176 0 2.875 −17.770 0.906 0.000 E.Epithelial 1.50E−97 1019 596 5.516 4.447 0.322 0.090 E.Epithelial 9.97E−20 2291 2385 4.475 4.737 0.168 0.210 E.Epithelial 1.31E−20 92 0 0.319 −17.770 0.568 0.000 E.Epithelial 3.64E−26 192 2 −0.274 −0.967 0.089 0.001 E.Epithelial  3.45E−129 1589 1154 2.248 1.581 0.184 0.084 E.Epithelial 1.41E−28 187 2 0.115 0.095 0.082 0.001 E.Epithelial 1.13E−18 216 38 0.980 1.343 0.073 0.017 E.Epithelial 1.65E−69 968 397 2.219 2.053 0.143 0.052 E.Epithelial 2.51E−24 211 2 2.524 −0.295 0.237 0.000 E.Epithelial 1.18E−19 1912 2023 4.445 4.668 0.129 0.159 E.Epithelial 2.04E−33 2270 2357 4.877 5.154 0.120 0.151 E.Epithelial 1.75E−31 2145 2278 4.760 5.076 0.129 0.171 E.Epithelial 3.26E−44 2081 2208 4.699 5.094 0.102 0.142 E.Epithelial 2.18E−30 2207 2280 5.026 5.375 0.107 0.141 E.Epithelial 2.42E−44 2268 2338 4.878 5.215 0.143 0.187 E.Epithelial 2.59E−38 2017 2167 4.476 4.837 0.140 0.193 E.Epithelial 4.00E−61 2269 2369 5.373 5.725 0.131 0.175 E.Epithelial 6.38E−50 2242 2331 5.044 5.451 0.124 0.170 E.Epithelial 2.02E−34 2100 2252 4.871 5.236 0.104 0.144 E.Epithelial 3.82E−50 1949 2130 4.329 4.688 0.124 0.174 E.Epithelial 5.00E−26 2265 2315 5.477 5.857 0.124 0.165 E.Epithelial 2.41E−19 1964 2089 4.239 4.440 0.119 0.146 E.Epithelial 1.81E−18 2057 2143 4.702 4.946 0.131 0.161 E.Epithelial 3.79E−29 2145 2242 4.599 4.880 0.137 0.174 E.Epithelial  1.29E−220 1772 1196 3.351 1.969 0.220 0.057 E.Epithelial  1.21E−164 2476 2461 6.627 5.634 0.380 0.190 E.Epithelial 6.89E−51 347 5 2.014 0.112 0.205 0.001 E.Epithelial 2.19E−40 1204 795 3.740 3.222 0.253 0.117 E.Epithelial 5.15E−51 1773 2001 3.174 3.549 0.133 0.194 E.Epithelial 3.60E−45 258 0 0.980 −17.770 0.778 0.000 E.Epithelial 3.58E−41 369 69 0.908 0.298 0.062 0.008 E.Epithelial 2.30E−59 800 206 1.653 0.915 0.134 0.021 E.Epithelial 2.32E−28 192 4 1.092 2.658 0.174 0.011 E.Epithelial 2.57E−24 208 7 0.762 0.119 0.067 0.001 E.Epithelial 1.26E−26 126 0 1.453 −17.770 0.302 0.000 E.Epithelial  1.97E−220 1135 105 2.030 1.996 0.071 0.006 E.Epithelial 1.56E−50 251 0 1.818 −17.770 0.505 0.000 E.Goblet 4.89E−19 65 49 1.932 1.652 0.043 0.027 E.Goblet 2.40E−42 109 106 4.608 2.874 0.104 0.031 E.Immature_Enterocytes  4.47E−116 179 1782 3.674 2.807 0.040 0.220 E.Immature_Enterocytes 5.85E−19 701 2422 5.364 4.770 0.063 0.144 E.Immature_Enterocytes 1.42E−64 531 1451 3.921 2.608 0.077 0.084 E.Immature_Enterocytes 1.25E−20 372 1685 2.473 2.669 0.028 0.144 E.Immature_Enterocytes 8.76E−34 114 62 1.042 0.714 0.073 0.031 E.Immature_Enterocytes 4.07E−23 48 3 0.678 0.057 0.032 0.001 E.Immature_Enterocytes 1.94E−63 141 36 3.999 2.544 0.338 0.032 E.Immature_Enterocytes 6.15E−44 175 153 2.143 1.137 0.129 0.056 E.Immature_Enterocytes 1.33E−48 613 2356 4.225 4.702 0.056 0.298 E.Immature_Enterocytes 5.39E−51 113 7 1.397 0.790 0.187 0.008 E.Immature_Enterocytes 1.17E−64 128 16 3.901 2.106 0.216 0.008 E.Immature_Enterocytes 1.97E−32 82 25 2.359 0.891 0.085 0.009 E.Immature_Enterocytes 1.53E−52 127 60 3.504 1.417 0.185 0.021 E.Immature_Enterocytes 4.29E−35 416 1093 2.099 1.521 0.039 0.069 E.Immature_Enterocytes 3.48E−19 698 2507 7.664 7.791 0.131 0.514 E.Immature_Enterocytes 1.55E−20 39 3 1.593 0.918 0.064 0.003 E.Immature_Enterocytes 3.01E−52 653 2426 4.807 5.516 0.027 0.166 E.Immature_Enterocytes 1.50E−22 43 0 0.817 −17.136 0.587 0.000 E.Immature_Enterocytes  5.26E−113 394 708 3.566 1.849 0.155 0.085 E.Immature_Enterocytes 1.32E−25 461 1230 2.604 2.094 0.060 0.112 E.Immature_Enterocytes 1.18E−21 568 1904 3.283 2.760 0.034 0.079 E.Immature_Enterocytes 1.59E−19 112 113 1.528 1.469 0.025 0.024 E.Immature_Enterocytes 2.24E−45 331 525 2.780 1.677 0.030 0.022 E.Immature_Enterocytes 2.90E−39 205 280 2.516 1.519 0.024 0.016 E.Immature_Enterocytes 3.79E−38 315 511 1.538 1.289 0.056 0.077 E.Immature_Enterocytes  5.49E−133 306 311 4.871 1.766 0.281 0.033 E.Immature_Enterocytes  1.03E−221 578 1299 4.124 2.429 0.307 0.213 E.Immature_Enterocytes 1.55E−19 657 2439 4.816 5.070 0.068 0.299 E.Immature_Enterocytes 2.54E−27 47 0 0.482 −17.136 0.070 0.000 E.Immature_Enterocytes 1.15E−51 0 335 −17.136 1.332 0.000 0.625 E.Immature_Enterocytes  9.59E−212 439 262 4.152 1.922 0.235 0.030 E.Immature_Enterocytes 2.37E−23 623 2345 4.161 4.603 0.068 0.350 E.Immature_Enterocytes 4.96E−46 316 506 2.507 1.988 0.090 0.100 E.Immature_Enterocytes 7.12E−44 110 35 3.715 0.764 0.051 0.002 E.Immature_Enterocytes 9.35E−60 312 458 2.565 1.514 0.086 0.061 E.Immature_Enterocytes  1.71E−139 418 656 3.543 1.786 0.086 0.040 E.Immature_Enterocytes 3.42E−66 716 2486 7.092 6.015 0.162 0.267 E.Immature_Enterocytes 3.74E−55 95 0 2.752 −17.136 0.125 0.000 E.Immature_Enterocytes  1.68E−293 437 130 3.542 0.830 0.295 0.013 E.Immature_Enterocytes 9.40E−35 257 450 1.832 1.332 0.054 0.067 E.Immature_Enterocytes 3.60E−28 69 5 0.391 0.133 0.094 0.006 E.Immature_Enterocytes 8.23E−58 533 1225 4.159 3.311 0.155 0.198 E.Immature_Enterocytes 8.08E−36 411 1843 2.260 2.811 0.023 0.152 E.Immature_Enterocytes 1.67E−36 76 0 1.232 −17.136 0.475 0.000 E.Immature_Enterocytes 1.42E−32 93 73 1.567 0.190 0.040 0.012 E.Immature_Enterocytes 1.80E−75 242 378 3.974 1.646 0.168 0.052 E.Immature_Enterocytes  1.67E−126 382 317 3.326 1.579 0.116 0.029 E.Immature_Enterocytes 2.92E−21 37 3 2.374 0.303 0.214 0.004 E.Immature_Enterocytes 4.69E−59 99 0 2.355 −17.136 0.465 0.000 E.Immature_Goblet 1.08E−20 52 536 2.942 2.472 0.009 0.069 E.Immature_Goblet 6.12E−19 40 7 2.868 2.057 0.077 0.008 E.Immature_Goblet 2.18E−26 224 1027 3.912 4.587 0.024 0.173 E.Immature_Goblet 1.47E−19 239 1063 6.042 6.699 0.020 0.144 E.Immature_Goblet 9.16E−20 235 1046 4.949 5.517 0.025 0.162 E.Immature_Goblet  2.65E−100 191 95 3.178 1.753 0.135 0.025 E.Immature_Goblet 5.94E−63 136 60 4.142 1.956 0.083 0.008 E.Immature_Goblet 3.89E−23 76 56 2.986 2.331 0.099 0.046 E.Secretory 4.32E−21 71 55 1.881 1.575 0.046 0.029 E.Secretory 4.04E−44 217 768 6.071 3.721 0.082 0.057 E.Secretory_All 5.43E−56 186 1439 2.490 2.417 0.020 0.150 E.Secretory_All 2.17E−20 257 376 0.761 1.187 0.025 0.049 E.Secretory_All 1.95E−34 92 12 0.381 0.262 0.053 0.006 E.Secretory_All 3.44E−22 44 0 0.224 −17.009 0.715 0.000 E.Secretory_All 2.15E−60 617 2286 4.044 4.617 0.051 0.284 E.Secretory_All 1.29E−35 447 968 2.042 1.769 0.041 0.074 E.Secretory_All 4.55E−28 96 38 1.493 1.517 0.064 0.026 E.Secretory_All 1.86E−29 66 2 1.578 −0.049 0.076 0.001 E.Secretory_All 7.64E−24 581 2105 4.109 4.548 0.046 0.226 E.Secretory_All 3.99E−28 566 1507 4.011 4.091 0.119 0.335 E.Secretory_All 2.66E−33 527 1389 2.622 2.603 0.058 0.151 E.Secretory_All 6.46E−21 304 1213 1.453 2.328 0.016 0.119 E.Secretory_All 1.58E−22 45 0 0.572 −17.009 0.882 0.000 E.Secretory_All 6.42E−30 660 2383 5.048 5.494 0.070 0.344 E.Secretory_All 8.95E−72 256 122 3.104 2.914 0.078 0.032 E.Secretory_All 5.50E−26 262 526 5.573 4.918 0.104 0.133 E.Secretory_All 1.60E−25 43 0 2.332 −17.009 0.780 0.000 E.Secretory_All 1.71E−19 665 2372 4.094 4.443 0.048 0.220 E.Secretory_All 9.73E−21 239 355 1.705 2.202 0.043 0.090 E.Secretory_All 2.04E−27 668 2378 5.856 6.413 0.042 0.219 E.Secretory_All 1.86E−19 657 2349 4.978 5.365 0.047 0.221 E.Secretory_All 8.54E−20 634 2261 5.035 5.410 0.055 0.254 E.Secretory_All 8.90E−27 679 2377 5.780 6.265 0.049 0.240 E.Secretory_All 2.24E−22 614 2156 4.810 5.301 0.042 0.207 E.Secretory_All 8.45E−40 658 2291 4.915 5.454 0.052 0.262 E.Secretory_All 7.52E−22 594 2062 4.443 4.892 0.050 0.236 E.Secretory_All 3.10E−27 654 2331 5.584 5.985 0.053 0.251 E.Secretory_All 5.76E−36 656 2277 5.725 6.412 0.045 0.249 E.Secretory_All 3.35E−30 654 2294 5.129 5.662 0.048 0.243 E.Secretory_All 1.46E−31 574 2063 4.392 4.898 0.048 0.243 E.Secretory_All 9.71E−22 671 2351 5.513 6.014 0.047 0.234 E.Secretory_All 3.28E−45 513 1284 2.627 2.022 0.055 0.090 E.Secretory_All 7.95E−26 59 7 1.212 3.224 0.101 0.049 E.Secretory_All 3.78E−26 84 31 0.817 1.254 0.037 0.018 E.Secretory_All  2.16E−111 367 190 1.991 2.936 0.029 0.029 E.Secretory_All 1.06E−20 53 8 0.507 0.705 0.043 0.007 E.Secretory_TA 6.93E−34 67 762 2.016 1.736 0.006 0.060 E.Secretory_TA 3.58E−31 205 948 5.003 3.805 0.070 0.141 E.Secretory_TA 7.63E−24 182 659 1.193 0.989 0.017 0.052 E.Secretory_TA 2.51E−21 31 0 0.852 −15.563 0.481 0.000 E.Secretory_TA 1.39E−29 55 2 1.518 −0.493 0.059 0.001 E.Secretory_TA 2.58E−19 93 112 −0.123 0.144 0.011 0.017 E.Secretory_TA 1.04E−32 131 214 0.668 0.288 0.024 0.030 E.Secretory_TA 1.78E−32 157 470 1.308 0.614 0.018 0.033 E.Secretory_TA 5.29E−32 123 829 1.015 1.932 0.007 0.084 E.Secretory_TA 7.34E−29 178 699 1.975 1.026 0.015 0.030 E.Secretory_TA 3.49E−40 170 385 1.717 0.423 0.040 0.037 E.Secretory_TA 9.81E−40 189 702 1.694 1.029 0.026 0.060 E.Secretory_TA 2.86E−24 85 50 2.785 0.438 0.044 0.005 E.Secretory_TA 3.26E−22 0 145 −15.563 0.302 0.000 0.258 E.Secretory_TA 1.65E−86 190 174 2.626 1.649 0.167 0.078 E.Secretory_TA 4.15E−41 151 465 1.456 0.576 0.020 0.033 E.Secretory_TA 1.04E−59 137 164 3.663 0.951 0.068 0.012 E.Secretory_TA 1.60E−31 196 820 2.335 1.556 0.020 0.050 E.Secretory_TA  6.08E−101 174 85 2.445 0.603 0.088 0.012 E.Secretory_TA 3.13E−27 48 0 1.467 −15.563 0.092 0.000 E.Secretory_TA 1.96E−28 95 45 −0.018 −0.222 0.030 0.012 E.Secretory_TA 1.35E−32 175 597 1.434 0.739 0.021 0.045 E.Secretory_TA 7.74E−26 44 2 1.126 −1.075 0.093 0.001 E.Stem 2.50E−23 74 148 3.162 1.471 0.031 0.019 E.Stem 8.44E−50 85 70 2.597 1.657 0.088 0.038 E.Stem 2.94E−23 74 179 2.280 0.755 0.037 0.031 F.Crypt 1.98E−19 20 0 1.954 −16.921 0.283 0.000 F.Crypt 1.56E−18 327 2176 5.041 4.216 0.024 0.089 F.Crypt 7.18E−31 97 192 5.654 4.084 0.057 0.038 F.Crypt 2.16E−22 233 1232 3.855 2.862 0.051 0.134 F.Crypt 9.05E−43 113 147 3.698 2.610 0.070 0.043 F.Crypt_hiFos 3.60E−23 75 694 3.780 4.902 0.016 0.331 F.Crypt_hiFos 1.05E−27 47 35 3.524 2.199 0.034 0.010 F.Crypt_loFos_1 4.61E−19 43 66 3.554 2.123 0.030 0.017 F.Crypt_loFos_2 3.84E−29 110 615 6.214 7.384 0.041 0.519 F.Crypt_loFos_2 5.18E−29 62 33 6.053 4.850 0.052 0.012 F.Endothelial 2.78E−21 47 1 0.968 0.308 0.086 0.001 F.Endothelial 2.27E−51 376 555 4.040 2.994 0.103 0.074 F.Endothelial 4.73E−23 305 316 3.545 3.217 0.062 0.052 F.Endothelial 8.95E−19 454 831 4.686 4.120 0.060 0.074 F.Endothelial 1.15E−28 472 972 5.206 5.921 0.064 0.218 F.Endothelial 1.54E−23 484 968 5.303 5.938 0.073 0.225 F.Endothelial 4.82E−22 382 648 4.926 4.096 0.106 0.101 F.Endothelial 1.53E−55 219 74 4.257 4.980 0.052 0.029 F.Endothelial 1.16E−30 434 739 4.965 3.807 0.042 0.032 F.Endothelial 3.80E−21 103 46 5.034 4.605 0.152 0.050 F.Endothelial 2.17E−22 400 640 4.404 3.357 0.129 0.100 F.Endothelial 7.96E−35 457 805 4.862 4.155 0.135 0.146 F.Fibroblast 1.32E−19 49 7 2.706 2.526 0.273 0.034 F.Fibroblast 5.35E−28 117 45 2.743 2.323 0.093 0.027 F.Fibroblast 1.48E−40 717 1585 3.721 3.260 0.162 0.260 F.Fibroblast 1.94E−31 168 113 2.089 2.273 0.099 0.076 F.Fibroblast 6.14E−32 69 0 3.069 −17.109 0.919 0.000 F.Fibroblast 2.59E−21 38 0 1.956 −17.109 0.315 0.000 F.Fibroblast 1.69E−35 66 0 1.718 −17.109 0.440 0.000 F.Fibroblast 2.36E−77 364 256 4.988 4.375 0.110 0.051 F.Fibroblast 2.38E−24 45 0 1.883 −17.109 0.439 0.000 F.Fibroblast 1.77E−62 295 201 3.026 2.214 0.157 0.061 F.Fibroblast 1.98E−32 910 2319 5.271 4.805 0.085 0.157 F.Fibroblast 6.46E−21 888 2397 4.993 5.369 0.069 0.243 F.Fibroblast 4.59E−28 657 1933 3.324 3.809 0.044 0.180 F.Fibroblast 8.74E−31 920 2340 5.419 4.709 0.093 0.144 F.Fibroblast 6.10E−29 105 55 2.990 2.114 0.148 0.042 F.Fibroblast 5.39E−24 43 0 2.835 −17.109 0.727 0.000 F.Fibroblast  6.38E−130 891 2100 5.637 4.077 0.308 0.246 F.Glia 2.11E−30 47 207 6.097 4.677 0.063 0.104 F.Glia 4.60E−20 24 2 2.928 3.996 0.311 0.054 F.Pcap_Venules 3.97E−23 168 163 4.186 3.081 0.060 0.027 F.Pcap_Venules 1.22E−28 125 31 2.471 1.782 0.205 0.032 F.Pcap_Venules 2.80E−20 195 215 4.447 3.783 0.141 0.098 F.Pcap_Venules 1.07E−26 135 61 2.764 1.834 0.106 0.025 F.Pcap_Venules 5.94E−32 151 66 3.759 2.793 0.208 0.047 F.Pcap_Venules 3.83E−23 111 31 3.011 2.740 0.085 0.020 F.Stromal 5.18E−27 60 0 2.677 −17.437 0.068 0.000 F.Stromal 1.53E−20 175 95 2.093 2.476 0.097 0.068 F.Stromal 5.21E−26 75 0 2.969 −17.437 0.926 0.000 F.Stromal 1.56E−30 335 261 2.621 2.292 0.150 0.093 F.Stromal 7.34E−28 67 0 1.704 −17.437 0.448 0.000 F.Stromal 5.18E−97 583 269 4.755 4.581 0.136 0.056 F.Stromal 1.14E−22 58 0 1.822 −17.437 0.503 0.000 F.Stromal 1.47E−22 358 309 4.532 4.779 0.137 0.140 F.Stromal 4.36E−19 1344 2379 4.908 5.246 0.094 0.211 F.Stromal 9.19E−29 1033 1928 3.279 3.731 0.063 0.161 F.Stromal 2.30E−29 1041 1451 3.919 3.291 0.113 0.102 F.Stromal 1.22E−29 1354 2268 5.288 4.642 0.119 0.128 F.Stromal 3.48E−30 1409 2367 5.497 4.938 0.126 0.143 F.Villus 8.61E−21 277 953 4.656 4.105 0.131 0.308 F.Villus 2.80E−31 230 508 4.183 3.868 0.077 0.137 F.Villus 2.35E−20 297 1189 6.482 5.598 0.114 0.247 F.Villus 1.13E−31 163 250 3.229 2.957 0.172 0.218 F.Villus 7.92E−55 288 1065 6.131 4.367 0.210 0.229 F.Villus_1 3.92E−22 102 210 4.101 3.592 0.042 0.061 F.Villus_1 9.12E−23 79 104 4.507 3.997 0.035 0.033 F.Villus_1 1.62E−34 116 440 6.109 4.030 0.130 0.117 F.Villus_2 2.22E−19 96 133 3.314 3.091 0.141 0.167 F.Villus_2 2.38E−21 172 625 6.146 4.565 0.151 0.183 I.Immune 1.55E−49 895 1415 3.606 3.541 0.155 0.235 I.Immune 4.26E−55 672 1082 7.127 7.775 0.201 0.507 I.Lymphoid 4.76E−42 891 1383 3.525 3.493 0.146 0.222 I.Lymphoid 1.56E−20 720 1058 4.300 4.512 0.141 0.241 I.Lymphoid 4.29E−19 119 15 1.892 2.304 0.121 0.020 I.Lymphoid 6.05E−38 703 1057 7.564 7.959 0.239 0.473 M.CD69pos_Mast 8.40E−22 189 255 4.288 4.007 0.221 0.246 M.CD69pos_Mast 8.92E−19 248 482 5.527 5.053 0.134 0.187 M.Macrophages 1.08E−21 405 1020 9.202 9.664 0.150 0.519 M.Mast 1.61E−22 70 16 3.561 3.432 0.083 0.017 M.Mast 9.61E−22 215 308 4.302 4.051 0.227 0.273 M.Mast 6.93E−23 276 538 5.537 5.010 0.145 0.196 M.Monocytes 2.42E−19 366 1237 3.727 3.459 0.082 0.230 M.Monocytes 1.27E−19 33 0 2.730 −16.729 0.829 0.000 M.Monocytes 3.80E−25 699 1775 7.238 7.798 0.145 0.543 M.Monocytes 4.59E−95 658 1743 5.981 6.943 0.106 0.549 M.Monocytes 3.47E−26 315 1208 3.733 3.629 0.066 0.235 M.Myeloid 1.39E−19 33 0 2.730 −17.202 0.831 0.000 M.Myeloid 2.35E−19 216 286 2.492 1.889 0.074 0.065 M.Myeloid 1.18E−18 708 2093 4.784 4.902 0.089 0.286 M.Myeloid 5.11E−31 816 1919 4.614 4.019 0.138 0.215 M.Myeloid 6.53E−22 538 967 4.008 3.606 0.136 0.185 M.Neutrophils 1.55E−28 139 101 5.153 6.964 0.039 0.100 M.Neutrophils 1.43E−23 130 78 6.818 4.463 0.238 0.028 T.Activated_CD4_hiFos 1.99E−22 186 396 5.084 4.054 0.072 0.075 T.Activated_CD4_loFos 9.55E−41 190 980 4.647 4.983 0.059 0.383 T.Activated_CD4_loFos 6.89E−24 175 459 5.409 4.321 0.081 0.099 T.Activated_CD4_loFos 5.79E−20 290 953 5.257 4.669 0.067 0.146 T.CD4 3.46E−27 609 1150 3.759 3.661 0.127 0.224 T.CD4 7.92E−21 259 116 2.939 3.015 0.134 0.063 T.CD4  8.80E−149 626 1712 4.589 4.983 0.122 0.437 T.CD4 2.96E−63 530 1299 5.073 5.153 0.137 0.354 T.CD4 3.71E−40 114 0 4.953 −17.403 0.824 0.000 T.CD4 5.26E−44 928 616 4.815 4.116 0.140 0.057 T.CD4 4.06E−29 141 15 2.266 3.009 0.098 0.017 T.CD4 1.69E−40 2004 2492 6.946 7.310 0.175 0.280 T.CD4 3.62E−22 2001 2488 6.447 6.696 0.171 0.252 T.CD4 1.73E−31 1995 2475 6.126 6.468 0.177 0.278 T.CD4 2.34E−22 1998 2479 6.362 6.628 0.162 0.241 T.CD4 4.29E−24 2003 2482 6.476 6.819 0.170 0.267 T.CD4 2.99E−38 1980 2449 5.861 6.212 0.173 0.273 T.CD4 2.10E−23 1994 2483 6.313 6.585 0.175 0.264 T.CD4 2.54E−24 1706 1943 4.685 4.416 0.284 0.268 T.CD4 7.99E−42 842 1536 3.807 4.013 0.098 0.206 T.CD8 2.23E−29 367 1396 3.958 4.457 0.067 0.359 T.CD8 3.71E−36 743 1473 4.015 3.854 0.232 0.411 T.CD8 1.19E−29 538 1501 3.494 3.896 0.040 0.146 T.CD8 2.16E−19 526 1484 4.204 4.593 0.065 0.242 T.CD8 1.42E−21 103 42 2.723 2.616 0.140 0.053 T.CD8 1.04E−23 975 2294 6.012 5.688 0.138 0.259 T.CD8 1.57E−21 973 2371 5.696 6.100 0.084 0.272 T.CD8 1.08E−25 936 2301 4.784 5.147 0.071 0.225 T.CD8 1.68E−24 891 1994 4.868 4.412 0.121 0.198 T.CD8 7.49E−20 97 54 2.923 2.770 0.098 0.049 T.CD8 2.30E−24 577 1701 3.863 4.309 0.084 0.338 T.CD8_IELs 3.52E−37 107 163 4.332 3.519 0.139 0.121 T.CD8_LP 2.38E−28 234 831 4.205 4.712 0.058 0.291 T.CD8_LP 4.36E−22 213 272 3.785 3.279 0.226 0.203 T.CD8_LP 1.85E−19 369 644 4.183 3.900 0.269 0.386 T.CD8_LP 4.74E−19 222 336 5.037 4.217 0.081 0.070 T.Cycling_T 2.46E−20 62 14 2.621 2.705 0.098 0.024 T.Memory_CD4 2.79E−42 92 565 4.414 4.883 0.031 0.260 T.Memory_CD4 1.37E−20 63 382 5.277 5.550 0.031 0.224 T.Memory_CD4 7.19E−20 46 3 3.185 2.559 0.426 0.018 T.Tcells 5.36E−55 812 1376 3.860 3.792 0.162 0.261 T.Tcells 6.96E−51 876 1412 4.448 4.659 0.170 0.318 T.Tcells 1.93E−24 197 39 2.531 2.768 0.122 0.029 T.Tcells 3.60E−29 96 0 4.859 −17.752 0.889 0.000 T.Tcells 2.08E−26 137 10 2.331 2.875 0.093 0.010 T.Tcells 1.80E−35 2108 1886 4.624 4.310 0.319 0.230 T.Tcells 3.25E−32 2495 2521 7.967 8.342 0.220 0.289 T.Tcells 7.65E−27 1195 1589 3.861 3.944 0.129 0.182 T.Tregs 1.68E−33 327 277 4.124 3.647 0.212 0.129 T.Tregs 8.45E−27 264 166 3.660 3.334 0.273 0.137 T.Tregs 7.35E−24 245 145 3.525 3.280 0.306 0.153

TABLE 14 Inflamed vs Non-Inflamed Markers ident gene coefD pvalD coefC pvalC mastfc pvalH B.Bcells ACTG1 0.270 5.04E−02 7.92E−01 7..87E−37  0.683 1.86E−36 B.Bcells ALOX5AP 1.113 2.65E−23 4.41E−01 5.15E−06 1.206 1.03E−26 B.Bcells ARHGDIB 0.388 2.70E−04 6.71E−01 2.39E−31 0.794 4.64E−33 B.Bcells ARPC1B 0.579 3.83E−10 7.39E−01 5.22E−31 0.862 2.35E−38 B.Bcells ARPC5 0.667 7.21E−13 5.39E−01 4.36E−19 0.581 3.26E−29 B.Bcells CD52 0.369 3.12E−05 7.63E−01 2.40E−21 0.733 4.94E−24 B.Bcells CD53 0.583 1.33E−10 8.15E−01 2.47E−42 0.665 4.66E−50 B.Bcells CFL1 0.234 1.10E−01 7.65E−01 1.27E−41 0.640 6.06E−41 B.Bcells CORO1A 0.567 8.48E−10 7.67E−01 4.11E−26 0.952 3.68E−33 B.Bcells COTL1 0.656 9.48E−13 6.51E−01 1.10E−15 0.881 9.67E−26 B.Bcells DHRS9 2.253 1.67E−38 6.91E−01 2.03E−04 0.667 2.75E−40 B.Bcells EVL 0.637 7.66E−11 5.01E−01 8.00E−15 0.598 5.05E−23 B.Bcells GAPDH 0.703 6.02E−05 7.07E−01 2.86E−40 1.072 1.53E−42 B.Bcells HLA-DMA 0.623 3.76E−12 5.61E−01 3.07E−18 0.742 1.13E−27 B.Bcells HLA-DPA1 0.341 3.29E−04 7.53E−01 2.61E−17 0.886 4.45E−19 B.Bcells HLA-DPB1 0.518 4.22E−09 7.06E−01 3.94E−12 1.223 1.12E−18 B.Bcells HLA-DQA1 0.464 1.19E−07 7.19E−01 3.46E−17 0.918 3.04E−22 B.Bcells HLA-DRB1 0.411 6.00E−06 9.67E−01 2.71E−20 1.120 1.13E−23 B.Bcells IGHA1 −0.818 2.00E−13 −1.76E+00  1.66E−33 −1.536 4.75E−44 B.Bcells IGHA2 −1.021 2.10E−29 −4.84E−01  1.07E−03 −0.548 1.41E−30 B.Bcells IGJ −0.595 2.67E−09 −1.53E+00  6.12E−33 −0.735 1.89E−39 B.Bcells IRF8 1.119 1.27E−25 4.66E−01 2.46E−09 0.595 3.17E−32 B.Bcells ITGB2 0.919 5.59E−16 5.53E−01 8.84E−11 0.819 4.23E−24 B.Bcells JUN −0.878 2.18E−18 −4.02E−01  1.80E−10 −0.519 3.57E−26 B.Bcells LAPTM5 0.556 2.49E−10 7.54E−01 1.55E−24 0.900 4.07E−32 B.Bcells LCP1 0.940 1.74E−19 3.73E−01 3.02E−07 0.635 3.99E−24 B.Bcells LMO2 2.231 1.51E−26 1.92E−01 2.88E−01 0.531 1.16E−25 B.Bcells UCP2 0.650 4.07E−13 5.08E−01 3.28E−15 0.592 1.24E−25 B.Cycling ACTB 0.439 6.44E−01 1.99E+00 1.93E−21 2.038 2.09E−20 B.Cycling HMGB1 1.804 5.95E−04 1.28E+00 4.98E−17 2.065 1.46E−18 B.Cycling HMGN2 1.138 8.01E−03 1.45E+00 3.95E−21 1.203 1.40E−21 B.FO PFN1 0.359 1.82E−01 9.87E−01 1.32E−24 1.005 7.00E−24 B.Plasma IGHA1 −0.203 3.71E−01 −1.88E+00  3.28E−37 −1.279 3.53E−36 B.Plasma IGJ −0.360 1.15E−01 −1.55E+00  2.98E−43 −0.787 1.49E−42 E.Absorptive CXCL1 1.378 3.33E−12 1.76E+00 1.91E−09 0.526 4.37E−19 E.Absorptive GSN 0.716 1.02E−03 8.13E−01 3.03E−25 0.533 1.80E−26 E.Absorptive HLA-DRB1 1.345 4.90E−18 9.64E−01 3.85E−11 2.221 1.76E−26 E.Absorptive RARRES3 0.801 1.82E−07 6.14E−01 1.42E−22 0.858 2.16E−27 E.Absorptive REG4 1.946 1.69E−19 4.60E−01 2.56E−01 0.505 1.02E−18 E.Absorptive S100A11 0.628 1.59E−04 9.39E−01 3.68E−22 0.966 3.62E−24 E.Absorptive_All CXCL1 1.593 8.90E−30 1.30E+00 1.79E−09 0.579 1.76E−36 E.Absorptive_All FOSB −1.301 4.06E−32 −6.54E−02  3.47E−01 −0.603 3.89E−31 E.Absorptive_All HLA-DRB1 0.979 3.64E−28 8.31E−01 7.00E−14 1.658 3.38E−39 E.Absorptive_All RBPMS 2.383 1.48E−22 2.24E−01 3.62E−01 0.951 1.21E−21 E.Absorptive_All S100A11 0.495 6.82E−08 6.73E−01 1.37E−27 0.763 9.01E−33 E.Absorptive_All S100A7 4.547 7.36E−19 1.00E+00 3.200 7.36E−19 E.Absorptive_All S100A9 1.871 1.30E−27 1.27E+00 3.26E−06 0.910 3.54E−31 E.Absorptive_All SOCS1 1.163 9.71E−15 7.36E−01 9.29E−09 0.521 6.59E−21 E.Absorptive_All TIMP1 1.310 5.00E−36 4.23E−01 2.36E−04 1.458 9.17E−38 E.Absorptive_TA_2 FOS −1.880 5.78E−18 −3.44E−01  4.50E−03 −1.292 1.12E−18 E.Absorptive_TA_2 MUC12 2.134 1.50E−19 8.02E−01 1.48E−17 0.648 2.77E−34 E.Absorptive_TA_2 PRAC1 4.156 3.34E−65 −3.64E−01  3.07E−05 0.675 1.21E−67 E.Absorptive_TA_2 RP11-708H21.4 −4.967 1.18E−22 1.00E+00 3.217 1.18E−22 E.Cycling_TA MUC12 1.573 1.73E−09 6.38E−01 2.92E−13 0.606 3.64E−20 E.Cycling_TA PRAC1 4.651 9.03E−79 −8.12E−01  1.67E−18 1.017 3.97E−94 E.Enterocyte_Immature_2 MUC12 1.674 7.19E−09 1.16E+00 1.13E−36 0.584 9.65E−43 E.Enterocyte_Immature_2 S100A11 1.180 9.06E−07 9.33E−01 3.01E−20 1.632 2.03E−24 E.Enterocytes C4orf3 0.792 6.34E−05 7.19E−01 6.37E−18 0.632 2.34E−20 E.Enterocytes PSME2 1.231 3.38E−05 7.97E−01 1.37E−19 1.177 2.92E−22 E.Enterocytes RARRES3 0.990 1.09E−03 6.33E−01 5.35E−18 0.954 2.83E−19 E.Enterocytes S100A11 1.304 2.80E−10 1.59E+00 2.99E−21 2.035 8.12E−29 E.Epithelial CXCL1 1.347 4.30E−21 1.45E+00 5.43E−13 0.681 2.57E−31 E.Epithelial FOSB −1.273 1.00E−27 −1.49E−01  1.64E−02 −0.573 7.74E−28 E.Epithelial MMP7 4.654 5.46E−27 1.00E+00 2.888 5.46E−27 E.Epithelial RBPMS 2.173 1.61E−19 1.78E−01 3.76E−01 0.988 1.25E−18 E.Epithelial S100A11 0.488 1.28E−05 6.56E−01 1.03E−29 0.760 1.07E−32 E.Epithelial S100A9 1.738 5.54E−20 8.89E−01 1.70E−03 0.843 4.67E−21 E.Epithelial SOCS1 1.325 2.37E−16 6.41E−01 1.01E−06 0.713 1.60E−20 E.Epithelial TIMP1 1.536 4.81E−41 3.71E−01 4.52E−04 1.705 1.73E−42 E.Immature_Enterocytes CXCL1 2.078 2.05E−28 1.48E+00 2.50E−06 1.034 4.41E−32 E.Immature_Enterocytes HLA-DRB1 0.924 1.72E−17 6.09E−01 1.44E−05 1.336 1.52E−20 E.Immature_Enterocytes PPP1R14A −2.410 1.12E−20 −6.04E−01  6.20E−02 −0.741 2.31E−20 E.Immature_Enterocytes S100A11 0.547 9.26E−07 5.89E−01 1.07E−15 0.771 6.43E−20 E.Immature_Enterocytes S100A6 2.392 1.87E−02 5.95E−01 6.29E−19 1.944 4.46E−19 E.Immature_Enterocytes S100A9 1.532 3.65E−15 1.52E+00 1.20E−07 0.650 2.99E−20 E.Secretory_All TIMP1 1.089 1.83E−23 2.08E−01 4.67E−02 1.093 3.21E−23 E.Secretory_TA PRAC1 4.571 2.02E−60 −5.40E−01  8.66E−07 0.941 2.32E−64 E.Stem PRAC1 3.706 7.35E−23 −3.74E−01  2.63E−03 0.554 9.92E−24 F.Fibroblast TIMP1 0.593 1.59E−04 8.03E−01 8.36E−35 0.649 1.04E−36 M.Monocytes RGS1 −1.005 1.10E−18 −2.29E−01  1.01E−02 −0.504 4.50E−19 T.CD4 TPT1 −0.473 4.86E−03 −3.97E−01  1.05E−18 −0.529 2.23E−19 ident n ref_n mu ref_mu total ref_total B.Bcells 1088 784 4.568 3.684 0.356 0.139 B.Bcells 363 113 2.490 2.404 0.267 0.078 B.Bcells 996 698 3.365 2.788 0.324 0.152 B.Bcells 830 483 3.223 2.507 0.308 0.109 B.Bcells 727 376 2.578 2.122 0.318 0.120 B.Bcells 738 489 4.554 4.249 0.454 0.243 B.Bcells 843 509 3.015 2.089 0.511 0.163 B.Bcells 1103 803 4.002 3.139 0.275 0.110 B.Bcells 878 553 3.954 3.425 0.459 0.200 B.Bcells 579 280 3.274 2.800 0.266 0.093 B.Bcells 251 22 2.056 1.627 0.644 0.042 B.Bcells 428 204 2.247 2.074 0.314 0.133 B.Bcells 1148 820 4.349 3.461 0.279 0.108 B.Bcells 777 433 2.966 2.496 0.330 0.133 B.Bcells 892 609 4.349 3.839 0.213 0.102 B.Bcells 756 458 4.753 4.354 0.218 0.100 B.Bcells 699 423 4.029 3.483 0.258 0.107 B.Bcells 824 526 5.128 4.513 0.238 0.099 B.Bcells 898 801 10.040 10.530 0.437 0.547 B.Bcells 586 660 7.980 8.085 0.447 0.541 B.Bcells 834 733 8.424 9.119 0.408 0.580 B.Bcells 427 131 2.748 2.460 0.564 0.142 B.Bcells 331 116 2.119 1.727 0.261 0.070 B.Bcells 773 714 3.640 4.069 0.271 0.337 B.Bcells 656 374 3.965 3.333 0.461 0.170 B.Bcells 416 150 2.374 2.251 0.418 0.138 B.Bcells 171 14 1.940 2.195 0.640 0.063 B.Bcells 627 319 2.674 2.286 0.385 0.150 B.Cycling 247 66 7.126 5.999 0.141 0.017 B.Cycling 244 56 4.953 4.301 0.270 0.040 B.Cycling 236 54 4.838 3.868 0.374 0.044 B.FO 331 301 5.213 4.171 0.123 0.054 B.Plasma 513 439 10.681 11.096 0.449 0.513 B.Plasma 509 441 8.796 9.454 0.403 0.551 E.Absorptive 98 41 4.137 2.399 0.299 0.037 E.Absorptive 339 478 3.011 2.206 0.150 0.121 E.Absorptive 294 279 2.895 1.786 0.022 0.010 E.Absorptive 298 365 2.781 2.203 0.173 0.142 E.Absorptive 100 25 3.802 2.852 0.194 0.025 E.Absorptive 259 294 3.764 2.592 0.098 0.049 E.Absorptive_All 231 62 3.762 2.713 0.414 0.054 E.Absorptive_All 266 494 1.325 1.467 0.038 0.078 E.Absorptive_All 620 396 3.145 1.983 0.048 0.014 E.Absorptive_All 103 10 3.442 2.027 0.438 0.016 E.Absorptive_All 774 714 3.645 3.004 0.201 0.119 E.Absorptive_All 58 0 2.227 −16.655 0.974 0.000 E.Absorptive_All 170 32 2.499 0.471 0.090 0.004 E.Absorptive_All 163 59 1.370 0.337 0.098 0.017 E.Absorptive_All 438 201 2.289 2.938 0.049 0.035 E.Absorptive_TA_2 179 306 1.859 2.794 0.012 0.041 E.Absorptive_TA_2 260 226 2.514 1.359 0.226 0.088 E.Absorptive_TA_2 263 144 2.341 2.749 0.310 0.225 E.Absorptive_TA_2 0 62 −14.615 −0.994 0.000 0.621 E.Cycling_TA 312 271 1.899 0.879 0.102 0.044 E.Cycling_TA 317 144 2.128 3.093 0.180 0.160 E.Enterocyte_Immature_2 239 274 3.756 2.470 0.346 0.163 E.Enterocyte_Immature_2 216 244 3.102 2.071 0.049 0.027 E.Enterocytes 175 142 1.501 0.868 0.050 0.026 E.Enterocytes 233 256 3.182 2.363 0.088 0.055 E.Enterocytes 235 270 3.016 2.530 0.176 0.144 E.Enterocytes 148 73 4.066 2.916 0.076 0.017 E.Epithelial 219 75 3.487 1.606 0.419 0.039 E.Epithelial 341 513 1.365 1.481 0.063 0.103 E.Epithelial 83 0 3.198 −16.298 0.976 0.000 E.Epithelial 101 13 0.301 1.545 0.078 0.024 E.Epithelial 770 683 3.325 2.826 0.198 0.124 E.Epithelial 140 32 1.890 −0.213 0.054 0.003 E.Epithelial 161 50 1.120 0.474 0.107 0.021 E.Epithelial 491 234 2.033 2.160 0.049 0.025 E.Immature_Enterocytes 128 30 3.901 2.461 0.218 0.019 E.Immature_Enterocytes 331 289 2.780 1.885 0.024 0.011 E.Immature_Enterocytes 8 123 1.439 2.462 0.003 0.108 E.Immature_Enterocytes 418 507 3.543 3.087 0.110 0.097 E.Immature_Enterocytes 716 1046 7.092 6.491 0.312 0.301 E.Immature_Enterocytes 95 34 2.752 0.286 0.064 0.004 E.Secretory_All 367 273 1.991 2.174 0.037 0.031 E.Secretory_TA 190 128 2.626 3.132 0.215 0.206 E.Stem 85 123 2.597 3.008 0.152 0.293 F.Fibroblast 891 857 5.637 4.449 0.515 0.218 M.Monocytes 315 434 3.733 3.747 0.206 0.286 T.CD4 1003 1101 5.109 5.533 0.222 0.327

TABLE 15 Non-inflamed vs Healthy Markers ident gene coefD pvalD coefC pvalC mastfc pvalH B.Bcells AC009501.4 −0.916 1.55E−31 −0.107 6.46E−02 −0.937 4.15E−31 B.Bcells ATP5E 0.717 3.01E−10 0.379 1.33E−21 0.759 3.93E−29 B.Bcells IGHA2 −0.527 3.04E−09 −2.008 1.75E−72 −0.743 9.22E−79 B.Bcells KLF6 0.650 7.92E−16 0.382 2.87E−13 0.510 2.17E−26 B.Bcells MT-ND3 0.607 7.92E−14 1.195 1.36E−44 0.881 1.81E−55 B.Bcells PTPRC 1.051 4.91E−27 0.155 2.46E−02 0.623 5.35E−27 B.Bcells RPL37 0.554 6.90E−04 0.717 1.27E−55 0.737 7.91E−57 B.Bcells RPL37A 0.455 1.21E−02 0.588 2.93E−41 0.620 2.14E−41 B.Bcells RPL39 0.601 1.10E−12 1.357 4.74E−68 0.777 1.04E−77 B.Bcells RPS21 0.504 6.05E−05 0.538 3.12E−33 0.581 1.52E−35 B.Bcells RPS29 0.650 2.45E−04 0.760 2.70E−44 1.063 5.70E−46 B.Bcells TPT1 0.749 1.23E−03 0.468 5.06E−34 0.893 4.18E−35 B.FO RPL39 0.886 1.90E−10 1.068 6.35E−19 0.825 1.11E−26 B.Plasma IGHA2 −2.624 3.65E−18 −1.896 5.43E−59 −1.489 4.45E−74 E.Absorptive AC009501.4 −1.463 4.21E−49 −0.120 8.47E−02 −1.284 1.77E−48 E.Absorptive HLA-B 0.270 4.72E−01 0.595 1.05E−24 0.590 1.06E−23 E.Absorptive MTRNR2L1 0.895 1.84E−19 1.658 4.14E−33 1.112 1.32E−49 E.Absorptive RARRES3 0.747 3.06E−14 0.347 1.38E−09 0.581 3.19E−21 E.Absorptive RPL39 0.677 2.87E−09 1.244 1.17E−39 0.626 4.26E−46 E.Absorptive_All AC009501.4 −1.264  7.06E−103 0.123 1.28E−03 −1.066  1.07E−103 E.Absorptive_All FTL −0.526 2.31E−04 −0.455 1.65E−33 −0.900 2.86E−35 E.Absorptive_All HLA-B 0.362 6.39E−04 0.449 2.48E−34 0.703 1.12E−35 E.Absorptive_All MTRNR2L1 0.785 2.86E−38 1.951 2.10E−98 0.999  2.59E−133 E.Absorptive_All RARRES3 0.675 2.18E−23 0.231 5.64E−06 0.516 9.20E−27 E.Absorptive_All REG4 1.752 3.37E−33 1.859 3.20E−11 0.815 1.39E−41 E.Absorptive_All S100A11 0.548 2.71E−17 0.545 1.55E−33 0.619 6.88E−48 E.Absorptive_All TIMP1 2.067 1.81E−50 0.866 5.73E−05 2.216 1.04E−52 E.Absorptive_TA_1 MTRNR2L1 1.146 8.46E−19 1.516 7.17E−15 1.172 6.75E−31 E.Absorptive_TA_2 AC009501.4 −1.739 2.56E−40 0.117 1.47E−01 −1.461 1.50E−39 E.Absorptive_TA_2 DDX5 0.525 1.79E−03 0.636 2.15E−21 0.544 1.98E−22 E.Absorptive_TA_2 IFITM3 0.720 2.42E−06 0.852 1.52E−22 0.710 2.80E−26 E.Absorptive_TA_2 LDHA 1.028 1.02E−05 0.611 1.09E−24 0.761 8.33E−28 E.Absorptive_TA_2 MTRNR2L1 0.757 4.60E−09 1.727 1.02E−21 0.900 4.28E−28 E.Absorptive_TA_2 PDIA3 1.141 4.53E−09 0.697 4.79E−36 0.613 2.59E−42 E.Absorptive_TA_2 S100A11 0.607 6.77E−03 0.723 4.50E−28 0.621 1.60E−28 E.Best4_Enterocytes RPL39 0.631 7.34E−04 1.861 4.91E−48 0.792 3.01E−49 E.Cycling_TA FN1 2.929 2.97E−19 1.569 1.55E−03 0.880 2.26E−20 E.Cycling_TA HLA-DMA 1.190 3.46E−16 0.628 1.63E−08 0.619 4.26E−22 E.Cycling_TA HLA-DRB1 1.763 2.23E−35 1.262 1.08E−13 2.259 3.56E−46 E.Cycling_TA LDHA 0.909 1.46E−03 0.590 1.40E−22 0.699 1.10E−23 E.Cycling_TA MTRNR2L1 0.929 7.85E−13 1.225 8.88E−13 0.969 5.82E−23 E.Cycling_TA PITX1 3.030 3.58E−24 0.562 4.71E−02 1.405 6.40E−24 E.Cycling_TA REG4 1.963 4.32E−33 1.134 1.47E−06 0.648 6.04E−37 E.Cycling_TA RPL38 −1.583 6.37E−05 0.661 5.53E−29 −0.562 2.63E−31 E.Cycling_TA S100A11 0.845 1.29E−03 0.879 8.92E−41 0.946 8.50E−42 E.Cycling_TA S100P 2.892 1.31E−66 1.107 1.75E−15 0.576 5.05E−79 E.Enterocyte_Immature_1 MTRNR2L1 0.847 1.93E−11 1.959 6.13E−27 0.960 1.38E−35 E.Enterocyte_Immature_1 MUC1 2.061 6.50E−29 1.062 3.51E−11 0.817 2.72E−37 E.Enterocyte_Immature_1 PLA2G2A 2.363 1.20E−33 1.177 1.84E−05 0.916 1.90E−36 E.Enterocyte_Immature_2 AC009501.4 −1.893 1.08E−44 −0.057 4.96E−01 −1.574 1.52E−43 E.Enterocyte_Immature_2 CYBA 0.963 4.30E−04 0.635 2.64E−22 1.235 6.61E−24 E.Enterocyte_Immature_2 MTRNR2L1 0.546 2.06E−05 2.221 7.06E−35 0.745 1.27E−37 E.Enterocyte_Immature_2 S100A11 1.196 1.16E−15 0.792 5.29E−21 1.325 7.45E−34 E.Enterocyte_Immature_2 S100P 3.046 4.72E−88 1.572 1.22E−42 0.691  2.49E−127 E.Enterocyte_Progenitor AC009501.4 −0.854 1.06E−13 0.590 4.97E−12 −0.577 4.42E−23 E.Enterocyte_Progenitor AGR2 1.071 3.71E−15 1.141 4.91E−29 0.796 2.57E−41 E.Enterocyte_Progenitor MTRNR2L1 0.728 8.62E−09 1.572 1.45E−16 0.795 9.74E−23 E.Enterocyte_Progenitor PLA2G2A 2.281 3.64E−63 1.180 1.13E−13 0.796 8.26E−74 E.Enterocyte_Progenitor REG4 2.664 1.23E−24 3.575 1.27E−11 1.488 1.76E−33 E.Enterocyte_Progenitor S100A11 0.971 2.84E−15 0.673 1.71E−13 1.012 4.59E−26 E.Enterocyte_Progenitor S100P 3.348 4.03E−89 0.786 1.07E−04 0.666 5.56E−91 E.Enterocyte_Progenitor TFF1 1.890 5.74E−23 1.734 2.85E−08 1.005 1.47E−28 E.Enterocyte_Progenitor TPT1 0.621 2.36E−04 0.665 1.18E−25 0.881 1.81E−27 E.Enterocytes AC009501.4 −1.866 1.23E−40 −0.142 1.36E−01 −1.561 6.81E−40 E.Enterocytes MDK 1.676 1.04E−12 0.471 5.07E−12 0.802 4.25E−22 E.Enterocytes MTRNR2L1 0.692 2.57E−07 2.089 4.41E−29 0.927 1.07E−33 E.Enterocytes MUC1 1.587 4.06E−23 1.250 4.29E−27 0.567 2.98E−47 E.Enterocytes PLA2G2A 1.809 2.99E−24 1.895 3.53E−16 0.692 1.41E−37 E.Epithelial AC009501.4 −1.108 9.77E−81 0.257 1.42E−11 −0.935 2.86E−89 E.Epithelial CXCL14 −0.921 9.13E−40 0.230 3.49E−02 −0.614 1.64E−39 E.Epithelial FTL −0.513 1.00E−04 −0.458 4.59E−33 −0.910 3.60E−35 E.Epithelial HLA-B 0.396 3.47E−04 0.443 1.30E−37 0.774 3.49E−39 E.Epithelial MT-ATP6 −1.097 1.66E−23 −0.006 8.87E−01 −0.895 2.08E−22 E.Epithelial MT-ND2 −1.167 2.79E−21 0.202 8.79E−08 −0.994 2.03E−26 E.Epithelial MTRNR2L1 0.850 9.20E−44 1.674 4.88E−82 0.679  1.89E−122 E.Epithelial RARRES3 0.620 4.04E−18 0.207 1.23E−04 0.628 2.79E−20 E.Epithelial S100A11 0.530 3.23E−15 0.618 1.52E−51 0.661 9.39E−64 E.Epithelial S100A6 0.301 2.31E−01 0.496 2.40E−45 0.516 2.09E−44 E.Epithelial TIMP1 1.540 5.11E−48 0.459 3.01E−04 1.551 1.36E−49 E.Goblet MT-ND3 0.498 7.33E−03 1.601 2.46E−32 0.739 1.01E−32 E.Immature_Enterocytes AC009501.4 −1.260 3.04E−65 0.211 4.27E−05 −1.018 1.51E−67 E.Immature_Enterocytes AGR2 0.728 3.16E−18 0.972 2.62E−53 0.555 1.76E−68 E.Immature_Enterocytes CYBA 0.445 1.33E−06 0.395 3.12E−19 0.603 2.98E−23 E.Immature_Enterocytes FTL −0.752 1.21E−05 −0.465 1.90E−20 −1.181 1.56E−23 E.Immature_Enterocytes IFITM3 0.915 9.50E−20 0.506 1.85E−06 0.883 1.26E−23 E.Immature_Enterocytes LCN2 1.886  9.90E−101 1.402 1.25E−41 0.625  5.65E−139 E.Immature_Enterocytes MTRNR2L1 0.695 7.45E−20 2.021 2.85E−66 0.874 5.30E−83 E.Immature_Enterocytes PLA2G2A 1.989  4.36E−103 1.457 6.45E−42 0.857  1.30E−141 E.Immature_Enterocytes REG4 1.956 1.41E−28 2.398 1.61E−13 0.746 2.99E−39 E.Immature_Enterocytes S100A11 0.955 5.32E−30 0.750 6.89E−33 1.131 7.95E−60 E.Immature_Enterocytes S100P 2.923  5.34E−176 1.278 3.65E−33 0.536  1.05E−205 E.Immature_Enterocytes SPINK1 1.222 9.55E−40 1.004 8.36E−30 0.632 1.90E−66 E.Immature_Enterocytes TPT1 0.539 2.35E−05 0.508 2.12E−42 0.772 4.75E−45 E.Immature_Goblet AGR2 2.345 6.20E−08 0.764 2.47E−16 1.709 1.12E−21 E.lmmature_Goblet TPT1 0.754 3.86E−02 0.643 2.05E−24 0.990 3.11E−24 E.Secretory LCN2 1.855 5.39E−27 1.240 2.36E−07 0.531 1.16E−31 E.Secretory MT-ND3 0.805 5.85E−10 1.765 4.64E−66 1.050 4.66E−73 E.Secretory_All AC009501.4 −1.150 1.41E−54 0.201 2.88E−04 −0.968 3.84E−56 E.Secretory_All FN1 3.218 2.44E−21 0.954 1.61E−01 0.852 1.10E−20 E.Secretory_All HLA-B 0.401 8.51E−03 0.538 1.96E−33 0.786 9.36E−34 E.Secretory_All LYZ 1.528 1.69E−40 0.007 9.67E−01 0.735 2.83E−39 E.Secretory_All MTRNR2L1 1.057 1.86E−42 1.178 3.07E−26 1.126 1.31E−65 E.Secretory_All TIMP1 1.285 2.27E−36 0.124 2.82E−01 1.065 2.01E−35 E.Secretory_TA AC009501.4 −1.585 8.94E−31 0.115 2.12E−01 −1.330 5.97E−30 E.Secretory_TA ITLN1 1.063 3.14E−05 1.247 4.03E−28 0.509 9.65E−31 E.Secretory_TA MTRNR2L1 0.865 2.67E−10 1.319 2.47E−13 0.940 4.99E−21 E.Secretory_TA SELK 0.530 8.31E−03 0.654 2.11E−28 0.531 9.05E−29 E.Secretory_TA TMEM258 0.859 7.78E−03 0.616 1.36E−32 0.505 5.93E−33 E.Stem FN1 2.880 3.19E−21 1.215 2.72E−03 0.920 4.28E−22 E.Stem MT-ND3 0.794 1.31E−01 2.049 1.10E−54 1.199 6.90E−54 E.Stem RPL38 0.661 4.33E−01 0.802 1.62E−26 0.721 1.61E−25 E.Stem RPL39 0.477 2.20E−01 2.093 3.68E−66 0.708 3.76E−65 E.Stem TPT1 1.665 1.60E−01 0.783 2.20E−24 2.134 1.06E−23 F.Crypt CAV1 1.146 6.66E−21 0.425 1.19E−03 0.542 4.16E−22 F.Crypt COX4I1 −0.620 5.73E−08 −0.433 1.89E−23 −0.556 9.59E−29 F.Crypt FOS 0.221 1.37E−02 0.779 1.66E−33 0.510 1.21E−33 F.Crypt HLA-A −0.858 3.01E−08 −0.421 4.76E−21 −0.885 1.22E−26 F.Crypt IFI27 −0.822 7.61E−24 −0.465 2.33E−09 −0.509 1.74E−30 F.Crypt MTRNR2L1 1.954 5.69E−89 1.365 1.03E−19 2.153  1.69E−105 F.Crypt TAGLN 1.641 6.57E−49 0.424 3.73E−03 0.610 1.82E−49 F.Crypt ZFP36 0.444 6.98E−08 0.650 5.22E−28 0.708 3.52E−33 F.Crypt_loFos_1 COL1A1 1.239 2.41E−07 0.734 4.28E−25 0.705 9.06E−30 F.Crypt_loFos_1 PRSS23 1.334 2.62E−19 0.656 2.20E−07 0.605 4.41E−24 F.Crypt_loFos_1 TAGLN 1.894 1.12E−27 0.488 3.84E−02 0.784 1.80E−27 F.Crypt_loFos_2 MTRNR2L1 2.286 6.13E−29 1.325 1.91E−04 2.508 8.21E−31 F.Endothelial MTRNR2L1 2.323 2.17E−63 0.404 7.42E−02 2.056 9.32E−63 F.Fibroblast C12orf75 1.496 7.49E−23 0.580 4.57E−05 0.520 2.30E−25 F.Fibroblast HLA-A −0.834 1.16E−10 −0.397 4.80E−28 −0.798 6.37E−36 F.Fibroblast MT-ND3 0.636 7.87E−21 0.470 2.89E−08 0.618 1.93E−26 F.Fibroblast MTRNR2L1 1.675  2.60E−106 1.221 4.14E−25 1.696  3.88E−128 F.Fibroblast PRSS23 1.294 2.72E−50 0.711 8.47E−16 0.612 4.42E−63 F.Fibroblast RPL12 −0.736 1.89E−05 −0.282 3.85E−18 −0.905 4.50E−21 F.Fibroblast RPL6 −0.596 4.05E−05 −0.302 1.03E−20 −0.723 2.68E−23 F.Fibroblast ZFP36 0.398 4.12E−10 0.492 1.11E−22 0.574 4.56E−30 F.Stromal COX4I1 −0.598 3.29E−14 −0.321 1.36E−22 −0.543 5.37E−34 F.Stromal HLA-A −0.702 1.63E−08 −0.431 3.40E−37 −0.748 6.50E−43 F.Stromal MT-ND3 0.674 9.33E−26 0.462 7.66E−09 0.646 7.06E−32 F.Stromal MTRNR2L1 1.682  8.15E−123 1.017 4.07E−20 1.568  1.14E−139 F.Stromal RPL12 −0.826 1.12E−09 −0.241 3.27E−15 −0.957 2.87E−22 F.Stromal RPL6 −0.475 9.80E−05 −0.296 5.70E−23 −0.646 3.61E−25 F.Villus COL3A1 1.208 3.13E−18 0.428 5.03E−13 0.713 1.60E−28 F.Villus DCN 1.226 4.58E−34 0.195 3.52E−02 0.911 7.65E−34 F.Villus LUM 1.197 5.30E−33 0.434 2.30E−04 0.865 9.06E−35 F.Villus MTRNR2L1 1.779 6.24E−54 0.986 2.13E−08 1.789 1.87E−59 F.Villus PRSS23 2.155 5.51E−22 0.943 9.10E−04 1.436 2.75E−23 F.Villus_1 LUM 1.625 2.01E−27 0.865 9.13E−05 1.631 1.31E−29 F.Villus_1 MTRNR2L1 2.150 5.43E−37 1.250 8.12E−06 2.357 4.13E−40 I.Immune AC009501.4 −0.932 5.84E−59 0.028 5.05E−01 −0.861 9.53E−58 I.Immune MT-ND3 0.681 6.43E−30 0.847 8.29E−29 0.764 1.08E−55 I.Lymphoid AC009501.4 −0.948 1.16E−60 −0.149 4.55E−04 −0.988 5.14E−62 I.Lymphoid MT-ND3 0.758 2.23E−37 0.926 2.61E−36 0.923 1.48E−70 I.Lymphoid RPL37 0.524 5.45E−11 0.503 1.44E−51 0.502 1.25E−59 I.Lymphoid RPL37A 0.491 2.75E−09 0.453 4.13E−45 0.530 1.54E−51 I.Lymphoid RPL39 0.827 8.12E−45 1.128 4.65E−71 0.655  1.50E−112 I.Lymphoid RPS29 0.637 9.51E−12 0.707 1.10E−75 0.781 2.12E−84 M.CD69pos_Mast RPL39 1.796 1.16E−28 0.968 1.14E−06 1.658 1.17E−32 M.Macrophages TPT1 0.714 8.54E−03 0.737 8.30E−33 0.974 3.94E−33 M.Mast RPL39 1.513 5.56E−24 0.951 2.55E−07 1.346 1.21E−28 M.Monocytes AC009501.4 −1.060 6.57E−29 0.372 1.03E−08 −0.841 7.05E−35 M.Monocytes MT-ND3 0.733 6.64E−13 0.813 1.66E−14 0.856 9.86E−25 M.Monocytes TPT1 0.556 2.12E−02 0.816 1.23E−66 0.828 1.88E−66 M.Myeloid AC009501.4 −0.944 2.00E−33 0.305 2.68E−07 −0.760 5.44E−38 M.Myeloid MT-ND3 0.917 2.08E−27 0.800 5.64E−18 0.988 1.77E−42 M.Myeloid RPL39 0.610 2.75E−13 1.381 1.80E−68 0.718 1.01E−78 M.Myeloid RPS29 0.600 7.49E−09 0.445 2.32E−17 0.811 1.40E−23 M.Myeloid TPT1 0.346 1.47E−02 0.601 5.47E−52 0.526 5.33E−52 T.Activated_CD4_hiFos KLRB1 1.024 1.50E−15 0.959 5.25E−20 0.684 9.27E−33 T.Activated_CD4_hiFos RPL39 0.774 2.49E−09 1.083 1.30E−16 0.673 2.62E−23 T.Activated_CD4_loFos ANXA1 −1.580 2.54E−20 −0.564 1.84E−10 −1.148 4.46E−28 T.Activated_CD4_loFos RPL39 0.795 1.80E−09 1.129 1.06E−18 0.758 1.66E−25 T.Activated_CD4_loFos RPS29 0.887 1.46E−03 0.801 2.45E−22 1.237 1.91E−23 T.CD4 AC009501.4 −0.753 4.11E−29 −0.129 1.39E−02 −0.760 2.82E−29 T.CD4 ANXA1 −0.895 1.22E−42 −0.535 1.27E−24 −0.730 3.47E−64 T.CD4 CCL5 −0.778 3.45E−32 −0.105 1.46E−01 −0.556 1.79E−31 T.CD4 MT-ND3 1.088 2.62E−57 0.642 6.53E−15 0.984 3.40E−69 T.CD4 RPL3 −0.728 2.37E−03 −0.318 1.54E−21 −1.038 1.83E−22 T.CD4 RPL37A 0.475 2.69E−07 0.411 7.65E−33 0.501 2.07E−37 T.CD4 RPL39 0.923 5.13E−44 1.004 2.72E−51 0.705 4.65E−92 T.CD4 RPS29 0.711 1.15E−10 0.647 6.11E−58 0.900 1.17E−65 T.CD8 AC009501.4 −1.089 1.99E−36 −0.001 9.93E−01 −0.985 3.16E−35 T.CD8 KLRB1 1.135 1.12E−34 1.051 7.19E−31 0.531 1.81E−62 T.CD8 RPL23 0.767 1.27E−16 0.346 2.23E−13 0.538 2.80E−27 T.CD8 RPL37 0.627 8.81E−08 0.482 7.49E−26 0.634 6.07E−31 T.CD8 RPL37A 0.826 4.47E−12 0.319 2.98E−12 0.847 1.05E−21 T.CD8 RPL38 0.718 1.08E−13 0.414 1.41E−19 0.667 1.65E−30 T.CD8 RPL39 1.033 5.50E−34 1.030 9.55E−35 0.907 1.25E−65 T.CD8 RPS29 0.843 3.90E−09 0.789 8.10E−50 1.202 4.48E−56 T.CD8_IELs KLRB1 1.786 3.21E−35 0.713 2.82E−08 1.362 1.01E−40 T.CD8_IELs RPL39 1.082 1.71E−15 1.055 1.63E−15 0.933 2.86E−28 T.CD8_IELs RPS29 0.856 1.86E−04 0.878 1.09E−24 1.294 1.31E−26 T.CD8_LP RPL39 0.992 8.30E−15 0.870 1.58E−10 0.842 1.06E−22 T.Memory_CD4 ANXA1 −1.046 1.67E−16 −0.708 7.68E−09 −0.987 9.99E−23 T.Memory_CD4 RPL39 1.077 5.94E−17 1.031 1.19E−16 0.931 7.91E−31 T.Memory_CD4 RPS29 0.892 7.88E−05 0.830 1.78E−24 1.253 9.46E−27 T.Tcells AC009501.4 −1.080 1.57E−72 −0.199 7.92E−06 −1.052 1.65E−75 T.Tcells MT-ND3 0.937 1.37E−53 0.698 2.96E−21 0.877 9.43E−72 T.Tcells RPL37 0.552 7.33E−12 0.504 1.21E−56 0.510 1.55E−65 T.Tcells RPL37A 0.695 1.59E−17 0.424 2.05E−41 0.689 6.00E−56 T.Tcells RPL38 0.691 8.14E−25 0.410 3.13E−37 0.533 5.34E−59 T.Tcells RPL39 0.917 7.15E−53 1.091 1.16E−73 0.692  3.64E−123 T.Tcells RPS16 0.532 6.76E−06 0.345 1.27E−33 0.549 7.74E−37 T.Tcells RPS23 0.460 7.92E−04 0.307 4.37E−24 0.604 2.01E−25 T.Tcells RPS29 0.688 3.71E−12 0.717 7.00E−89 0.868 5.80E−98 T.Tcells TMSB4X −0.761 2.25E−01 −0.421 6.54E−35 −1.006 4.87E−34 T.Tregs RPL39 1.289 3.69E−18 0.954 7.35E−09 1.110 2.23E−24 ident n ref_n mu ref_mu total ref_total B.Bcells 315 1399 1.732 2.300 0.021 0.136 B.Bcells 818 1847 2.717 2.347 0.060 0.105 B.Bcells 660 2002 8.085 9.053 0.126 0.750 B.Bcells 587 1098 2.563 2.360 0.089 0.144 B.Bcells 579 1094 4.387 3.127 0.075 0.059 B.Bcells 255 297 2.180 2.371 0.081 0.107 B.Bcells 885 2227 3.902 3.143 0.099 0.147 B.Bcells 893 2284 3.925 3.297 0.087 0.144 B.Bcells 670 1378 4.908 3.627 0.154 0.131 B.Bcells 845 2058 3.313 2.862 0.092 0.164 B.Bcells 895 2273 4.561 3.910 0.104 0.168 B.Bcells 910 2320 4.586 3.872 0.085 0.133 B.FO 262 482 5.527 4.678 0.117 0.120 B.Plasma 429 1319 8.601 9.410 0.134 0.720 E.Absorptive 232 1244 2.454 2.477 0.027 0.146 E.Absorptive 582 1639 5.319 4.978 0.070 0.156 E.Absorptive 294 473 5.538 4.723 0.135 0.124 E.Absorptive 365 675 2.203 2.124 0.082 0.144 E.Absorptive 388 741 3.887 1.713 0.069 0.029 E.Absorptive_All 1006 1770 3.283 2.771 0.162 0.200 E.Absorptive_All 2353 2409 5.065 5.477 0.107 0.146 E.Absorptive_All 2292 2228 4.721 4.370 0.148 0.113 E.Absorptive_All 1078 634 5.863 4.769 0.375 0.103 E.Absorptive_All 817 442 2.047 2.072 0.137 0.076 E.Absorptive_All 248 39 5.078 1.191 0.236 0.003 E.Absorptive_All 1368 957 2.892 2.147 0.143 0.060 E.Absorptive_All 372 37 2.660 0.887 0.045 0.001 E.Absorptive_TA_1 157 181 6.221 5.640 0.120 0.093 E.Absorptive_TA_2 164 978 2.742 2.209 0.024 0.099 E.Absorptive_TA_2 283 778 1.155 1.041 0.015 0.039 E.Absorptive_TA_2 290 723 1.776 1.210 0.021 0.035 E.Absorptive_TA_2 337 1020 2.353 1.774 0.046 0.093 E.Absorptive_TA_2 153 277 4.987 3.981 0.058 0.052 E.Absorptive_TA_2 315 869 2.000 1.269 0.051 0.084 E.Absorptive_TA_2 337 1031 2.441 1.900 0.035 0.073 E.Best4_Enterocytes 211 459 4.588 2.087 0.064 0.024 E.Cycling_TA 60 4 0.716 −0.174 0.035 0.001 E.Cycling_TA 175 168 −0.050 −0.238 0.015 0.013 E.Cycling_TA 225 187 1.706 0.621 0.011 0.004 E.Cycling_TA 329 1010 2.055 1.402 0.037 0.072 E.Cycling_TA 165 276 4.088 3.351 0.036 0.037 E.Cycling_TA 58 6 0.112 −0.939 0.029 0.001 E.Cycling_TA 127 71 3.274 −0.106 0.050 0.003 E.Cycling_TA 332 1148 3.594 3.094 0.056 0.137 E.Cycling_TA 335 1020 2.945 1.523 0.051 0.058 E.Cycling_TA 237 75 1.477 −0.225 0.056 0.005 E.Enterocyte_Immature_1 174 298 6.433 5.302 0.152 0.119 E.Enterocyte_Immature_1 96 50 3.275 1.480 0.141 0.021 E.Enterocyte_Immature_1 94 36 3.492 1.624 0.047 0.005 E.Enterocyte_Immature_2 157 980 3.004 2.688 0.027 0.133 E.Enterocyte_Immature_2 327 1036 3.316 2.784 0.036 0.079 E.Enterocyte_Immature_2 152 337 5.575 4.159 0.083 0.069 E.Enterocyte_Immature_2 244 455 2.071 0.909 0.021 0.018 E.Enterocyte_Immature_2 254 130 2.673 0.233 0.122 0.012 E.Enterocyte_Progenitor 168 730 3.904 2.797 0.054 0.109 E.Enterocyte_Progenitor 339 718 5.063 3.249 0.129 0.078 E.Enterocyte_Progenitor 149 247 6.112 5.395 0.111 0.112 E.Enterocyte_Progenitor 222 118 4.377 2.794 0.179 0.032 E.Enterocyte_Progenitor 60 12 6.281 1.470 0.176 0.001 E.Enterocyte_Progenitor 229 359 3.665 2.418 0.059 0.039 E.Enterocyte_Progenitor 197 33 3.042 1.938 0.130 0.010 E.Enterocyte_Progenitor 86 40 4.833 1.617 0.085 0.004 E.Enterocyte_Progenitor 348 974 4.387 3.701 0.037 0.064 E.Enterocytes 127 684 2.550 2.661 0.017 0.097 E.Enterocytes 304 670 2.972 2.497 0.139 0.221 E.Enterocytes 157 272 5.572 4.456 0.087 0.070 E.Enterocytes 129 100 2.732 0.805 0.142 0.029 E.Enterocytes 106 60 3.870 0.490 0.065 0.004 E.Epithelial 1040 1715 3.458 2.717 0.172 0.170 E.Epithelial 418 747 2.000 1.137 0.013 0.012 E.Epithelial 2313 2393 4.946 5.360 0.086 0.119 E.Epithelial 2303 2268 4.649 4.295 0.122 0.094 E.Epithelial 2165 2368 6.556 6.541 0.252 0.273 E.Epithelial 2214 2400 6.759 6.517 0.261 0.239 E.Epithelial 1065 596 5.621 4.447 0.362 0.090 E.Epithelial 739 397 1.841 2.053 0.084 0.052 E.Epithelial 1509 1196 3.018 1.969 0.149 0.057 E.Epithelial 2474 2461 6.133 5.634 0.269 0.190 E.Epithelial 569 105 2.584 1.996 0.052 0.006 E.Goblet 211 527 5.902 3.597 0.084 0.042 E.Immature_Enterocytes 459 1782 3.507 2.807 0.092 0.220 E.Immature_Enterocytes 817 1451 4.347 2.608 0.158 0.084 E.Immature_Enterocytes 852 1726 3.348 2.928 0.078 0.119 E.Immature_Enterocytes 1037 2426 5.064 5.516 0.052 0.166 E.Immature_Enterocytes 299 280 1.936 1.519 0.023 0.016 E.Immature_Enterocytes 529 311 3.748 1.766 0.223 0.033 E.Immature_Enterocytes 475 660 6.100 4.939 0.248 0.154 E.Immature_Enterocytes 500 262 3.949 1.922 0.233 0.030 E.Immature_Enterocytes 113 35 5.628 0.764 0.196 0.002 E.Immature_Enterocytes 530 656 3.071 1.786 0.079 0.040 E.Immature_Enterocytes 518 130 2.782 0.830 0.207 0.013 E.Immature_Enterocytes 422 378 3.014 1.646 0.150 0.052 E.Immature_Enterocytes 1002 2180 4.413 3.797 0.089 0.126 E.Immature_Goblet 344 969 6.360 5.245 0.206 0.268 E.lmmature_Goblet 338 981 4.883 4.192 0.048 0.087 E.Secretory 120 55 3.684 1.893 0.066 0.009 E.Secretory 398 768 6.215 3.721 0.166 0.057 E.Secretory_All 354 1439 2.920 2.417 0.052 0.150 E.Secretory_All 64 2 0.437 −0.049 0.033 0.001 E.Secretory_All 1088 2284 4.746 4.429 0.084 0.141 E.Secretory_All 268 122 1.816 2.914 0.033 0.032 E.Secretory_All 513 526 5.467 4.918 0.189 0.133 E.Secretory_All 314 190 2.285 2.936 0.030 0.029 E.Secretory_TA 126 762 1.989 1.736 0.012 0.060 E.Secretory_TA 301 818 4.563 3.164 0.153 0.158 E.Secretory_TA 154 259 4.454 3.805 0.043 0.046 E.Secretory_TA 278 720 1.320 1.046 0.026 0.057 E.Secretory_TA 303 877 1.944 1.608 0.044 0.102 E.Stem 63 6 1.178 −0.485 0.050 0.002 E.Stem 237 575 6.088 3.493 0.105 0.042 E.Stem 239 604 3.797 3.107 0.052 0.081 E.Stem 233 549 5.235 2.766 0.103 0.044 E.Stem 240 613 4.911 3.971 0.037 0.050 F.Crypt 162 148 3.001 2.403 0.101 0.061 F.Crypt 739 2049 3.273 3.686 0.049 0.180 F.Crypt 689 1621 5.550 4.853 0.183 0.266 F.Crypt 833 2285 4.229 4.750 0.059 0.231 F.Crypt 429 1470 3.041 3.819 0.027 0.157 F.Crypt 359 192 5.360 4.084 0.171 0.038 F.Crypt 238 147 3.168 2.610 0.102 0.043 F.Crypt 630 1331 4.625 4.035 0.163 0.228 F.Crypt_loFos_1 284 814 4.116 3.384 0.183 0.316 F.Crypt_loFos_1 129 147 2.980 1.974 0.106 0.060 F.Crypt_loFos_1 101 66 2.784 2.123 0.042 0.017 F.Crypt_loFos_2 88 33 6.193 4.850 0.081 0.012 F.Endothelial 226 74 4.910 4.980 0.085 0.029 F.Fibroblast 174 45 3.194 2.323 0.190 0.027 F.Fibroblast 1700 2351 4.642 5.131 0.129 0.249 F.Fibroblast 812 637 4.188 3.642 0.098 0.053 F.Fibroblast 723 256 5.408 4.375 0.293 0.051 F.Fibroblast 488 201 3.293 2.214 0.313 0.061 F.Fibroblast 1778 2426 4.932 5.216 0.137 0.227 F.Fibroblast 1750 2392 4.780 5.109 0.145 0.248 F.Fibroblast 1162 1237 4.547 4.098 0.237 0.185 F.Stromal 1791 1990 3.355 3.683 0.109 0.152 F.Stromal 2171 2366 4.816 5.330 0.167 0.261 F.Stromal 1025 630 4.241 3.673 0.128 0.053 F.Stromal 949 269 5.304 4.581 0.323 0.056 F.Stromal 2195 2397 4.831 5.095 0.150 0.197 F.Stromal 2183 2360 4.695 5.023 0.162 0.219 F.Villus 569 953 4.500 4.105 0.242 0.308 F.Villus 436 508 4.004 3.868 0.129 0.137 F.Villus 372 386 4.842 4.352 0.164 0.121 F.Villus 277 145 5.429 4.722 0.139 0.044 F.Villus 79 18 3.522 2.186 0.099 0.009 F.Villus_1 181 104 5.000 3.997 0.114 0.033 F.Villus_1 157 50 5.170 4.481 0.076 0.015 I.Immune 848 1415 3.516 3.541 0.138 0.235 I.Immune 1244 798 4.731 3.743 0.152 0.049 I.Lymphoid 800 1383 3.317 3.493 0.114 0.222 I.Lymphoid 1323 823 4.803 3.751 0.172 0.052 I.Lymphoid 2199 1983 4.285 3.752 0.239 0.149 I.Lymphoid 2218 2021 4.192 3.728 0.200 0.132 I.Lymphoid 1537 987 5.084 3.996 0.316 0.096 I.Lymphoid 2314 2141 5.089 4.344 0.286 0.158 M.CD69pos_Mast 145 96 5.003 4.035 0.059 0.020 M.Macrophages 354 936 5.437 4.616 0.069 0.103 M.Mast 160 115 4.935 3.926 0.062 0.022 M.Monocytes 273 1237 3.685 3.459 0.059 0.230 M.Monocytes 387 696 4.540 3.756 0.060 0.063 M.Monocytes 601 1679 5.546 4.538 0.109 0.151 M.Myeloid 321 1396 3.664 3.488 0.065 0.250 M.Myeloid 518 765 4.488 3.794 0.078 0.071 M.Myeloid 566 1047 4.766 3.594 0.142 0.117 M.Myeloid 785 1787 4.171 3.829 0.080 0.144 M.Myeloid 864 2173 5.316 4.525 0.120 0.175 T.Activated_CD4_hiFos 199 381 4.555 3.648 0.208 0.212 T.Activated_CD4_hiFos 210 396 5.055 4.054 0.079 0.075 T.Activated_CD4_loFos 220 980 4.314 4.983 0.054 0.383 T.Activated_CD4_loFos 201 459 5.305 4.321 0.086 0.099 T.Activated_CD4_loFos 298 953 5.264 4.669 0.069 0.146 T.CD4 453 1150 3.452 3.661 0.076 0.224 T.CD4 739 1712 4.319 4.983 0.119 0.437 T.CD4 514 1299 4.767 5.153 0.107 0.354 T.CD4 851 616 4.812 4.116 0.128 0.057 T.CD4 1562 2475 6.156 6.468 0.141 0.278 T.CD4 1408 1953 4.371 4.008 0.152 0.164 T.CD4 1009 918 5.245 4.426 0.232 0.120 T.CD4 1489 2118 5.240 4.704 0.198 0.195 T.CD8 213 1267 3.751 3.703 0.047 0.268 T.CD8 305 415 4.826 3.743 0.299 0.192 T.CD8 596 1318 3.743 3.374 0.101 0.174 T.CD8 689 1817 4.275 3.801 0.099 0.188 T.CD8 698 1775 4.113 3.818 0.078 0.162 T.CD8 622 1457 3.891 3.495 0.104 0.185 T.CD8 487 819 4.945 4.075 0.132 0.121 T.CD8 730 1994 5.173 4.412 0.123 0.198 T.CD8_IELs 148 163 4.141 3.519 0.169 0.121 T.CD8_IELs 191 399 4.975 4.012 0.072 0.077 T.CD8_IELs 274 907 5.291 4.350 0.069 0.118 T.CD8_LP 195 336 4.890 4.217 0.064 0.070 T.Memory_CD4 117 565 3.972 4.883 0.029 0.260 T.Memory_CD4 239 365 5.688 4.809 0.121 0.101 T.Memory_CD4 334 810 5.759 4.996 0.100 0.143 T.Tcells 652 1376 3.553 3.792 0.105 0.261 T.Tcells 1213 730 4.762 4.006 0.157 0.056 T.Tcells 1981 1945 4.445 3.975 0.228 0.161 T.Tcells 2000 1915 4.298 3.911 0.193 0.141 T.Tcells 1791 1560 3.983 3.609 0.229 0.154 T.Tcells 1410 940 5.156 4.167 0.290 0.097 T.Tcells 2149 2267 5.070 4.717 0.219 0.180 T.Tcells 2178 2344 5.307 5.022 0.209 0.185 T.Tcells 2106 2150 5.215 4.563 0.259 0.168 T.Tcells 2256 2521 7.939 8.342 0.195 0.289 T.Tregs 183 157 4.882 4.028 0.064 0.030

Example 18—STAR Methods Computational Analyses

Processing FASTQ reads into gene expression matrices. Cell Ranger v2.0 was used to demultiplex the FASTQ reads, align them to the hg19 human transcriptome, and extract their “cell” and “UMI” barcodes. The output of this pipeline is a digital gene expression (DGE) matrix for each sample, which records the number of UMIs for each gene that are associated with each cell barcode. DGE matrices were filtered to remove low quality cells, defined as cells in which fewer than 250 unique genes were detected. This cutoff was determined empirically: higher cutoffs led to disproportionate filtering of mast and T cells, whereas lower cutoffs did not affect the cell type distribution, but did reduce overall data quality. To account for differences in sequencing depth across cells, UMI counts were normalized by the total number of UMIs per cell and converted to transcripts-per-10,000 (henceforth “TPM”).

Cell clustering overview. To cluster single cells into distinct cell subsets, Applicants followed the general procedure outlined in with additional modifications. This workflow includes the following steps: partitioning cells into epithelial, stromal, and immune compartments; and clustering the cells within each compartment, which entails the selection of “variable” genes, batch correction, dimensionality reduction (PCA), and graph clustering. Each step of this workflow is explained in detail below.

Partitioning cells into epithelial, stromal, and immune compartments. Cells were partitioned into epithelial, stromal, and immune compartments based on the expression of known marker genes. First, Applicants clustered the cells within each sample by their gene expression profiles (with the clustering procedure below). The clusters were scored for the following gene signatures: epithelial cells (EPCAM, KRT8, KRT18), stromal cells (COL1A1, COL1A2, COL6A1, COL6A2, VWF, PLVAP, CDH5, S100B), and immune cells (CD52, CD2, CD3D, CD3G, CD3E, CD79A, CD79B, CD14, CD16, CD68, CD83, CSF1R, FCER1G). Signature scores were calculated as the mean log₂(TPM) across all genes in the signature. Each cluster was assigned to the compartment of its maximal score and all cluster assignments were manually inspected to ensure the accurate segregation of cells. Finally, the cells within each compartment were assembled into three DGE matrices, comprising all epithelial cells, all stromal cells, and all immune cells.

Variable gene selection. Applicants identified sets of variable genes, defined as genes with high variance of expression relative to their mean expression. To prevent “batch” differences between samples from unduly impacting these gene sets, Applicants performed variable gene selection separately for each sample, then merged the results to form a consensus variable gene list. To identify variable genes within a sample, Applicants first calculated the mean (μ) and the coefficient of variation (CV) of expression of each gene. Genes were then grouped into 20 equal-frequency bins (ventiles) according to their mean expression levels. LOESS regression was used to fit the relationship, log(CV)˜log(μ), and the 1,500 genes with the highest residuals were evenly sampled across these expression bins. After this procedure was performed for each sample, genes were ranked according to the number of samples from which they were recovered. A consensus set of 1,500 variable genes was then formed by selecting the genes with the greatest recovery rates across all samples and ties were broken by random sampling. This consensus gene set was then pruned through the removal of all ribosomal, mitochondrial, immunoglobulin, and HLA genes, which were found to induce unwanted batch effects in downstream clustering steps.

Batch correction. Applicants observed substantial variability between cells that had been obtained from different human subjects, which likely reflects a combination of technical and biological differences. In some cases, these “batch effects” led to cells clustering by patient or disease phenotype, rather than by cell type or cell state. To eliminate these batch differences, Applicants ran ComBat with default parameters on the log₂(TPM) expression matrix, allowing cells to be clustered by cell type or cell state. Importantly, these batch-corrected data were only used for the PCA and all steps relying on PCA (e.g. clustering, diffusion map, t-SNE visualization); all other analyses (e.g. differential expression analysis) were based on the original expression data.

Dimensionality reduction, graph clustering, and t-SNE visualization. Cells were clustered at two stages of the analysis: first, to initially partition the cells within each sample into epithelial, stromal, and immune compartments (single sample clustering), and second, to cluster cells from multiple samples into distinct subsets (multi sample clustering). For single-sample clustering, Applicants first ran PCA on the variable genes of the entire log₂(TPM) expression matrix. The Infomap graph clustering algorithm was then applied to the k-nearest neighbor (k-NN) graph defined using PCs 1 to 20 and k=50 nearest neighbors. These parameters were designed to “over-cluster” the cells, ensuring that cells from distinct compartments were not grouped together. In contrast, for multi-sample clustering, Applicants ran PCA on the variable genes of the batch-corrected expression matrix. Applicants then applied Phenograph to the k-NN graph defined using PCs 1 to 20 and a varying k, which was selected through close inspection of the data: k=750 for epithelial cells, k=500 for stromal cells, and k=500 for immune cells. Although most clusters were stable over a range of k, some rare epithelial cell subsets, such as tuft cells and M cells, were not well represented because they had been merged with larger clusters, requiring a higher granularity (k=750) and merged the clusters for the tuft cells, enteroendocrine cells, M cells, and BEST4⁺ enterocytes with the original clusters. In addition, Applicants partitioned the immune cells into myeloid, B cell, and T cell compartments, and repeated the clustering using the k-NN graph defined with PCs 1 to 15 and k=50 for myeloid cells, k=100 for B cells, and k=100 for T cells. Finally, the Barnes-Hut t-Distributed Stochastic Neighbor Embedding (t-SNE) algorithm was run on the PCs with perplexity=20 and for 10,000 iterations to produce a two-dimensional embedding of the data for visualization (FIG. 1B).

Differential expression analysis. Differential expression (DE) tests were performed using MAST, which fits a hurdle model to the expression of each gene, consisting of logistic regression for the zero process (i.e. whether the gene is expressed) and linear regression for the continuous process (i.e. the expression level). To reduce the size of the inference problem, separate models were fit for all levels of the cell tree, comparing cells within the given group to all other cells (e.g. ISCs vs. non-ISCs). The regression model includes terms to capture the effects of the cell subset and the disease state on gene expression, while controlling for cell complexity (i.e. the number of genes detected per cell).

Specifically, Applicants used the regression formula, Y_(i)˜X+D+N, where Y_(i) is the standardized log₂(TPM) expression vector for gene i across all cells, X is a binary variable reflecting cell subset membership (e.g. ISCs vs. non-ISCs), D is the disease state associated with each cell, and Nis the number of genes detected in each cell. Overall, Applicants fit three types of DE models, which varied by the encoded disease states: (1) to identify cell subset markers and DE genes in UC patients relative to healthy controls, Applicants used three disease states: Healthy, UC non-inflamed, and UC inflamed; (2) to identify DE genes between non-inflamed and inflamed patient samples, Applicants used two disease states: UC non-inflamed and UC inflamed; and (3) to identify genes that are specific to cell subsets in healthy subjects and UC patients, Applicants used two disease states: Healthy and UC. Additionally, a few heuristics were used to increase the speed of the tests: Applicants required all tested genes to be expressed by at least 1% of cells and to have a minimum fold change of 1.2 within the group of interest, and cells were evenly downsampled across groups so that a maximum of 2,500 cells were tested for each cell subset. In all cases, the discrete and continuous coefficients of the model were retrieved and p-values were calculated using the likelihood ratio test in MAST. Q-values were separately estimated for each cell subset comparison using the Benjamini-Hochberg correction. Unless otherwise indicated, all reported DE coefficients and q-values correspond to the discrete component of the model (i.e. the logistic regression).

Estimation of the droplet contamination rate and filtering of putative ambient RNA contaminants. Droplets encapsulate single cells with small portions of the extracellular environment, leading to low but persistent levels of contamination by ambient RNA [REF-Macosko]. To correct for this, Applicants explicitly modeled droplet contamination. First, Applicants partitioned individual cells into the following groups: epithelial cells, fibroblasts, endothelial cells, myeloid cells, B cells, and T cells. Applicants reasoned that each group should uniquely express a subset of genes that are not found in other cells; for example, B cells uniquely express IGHA1 and T cells uniquely express CD3D. Therefore, the off-target expression of such genes in the incorrect group (e.g. IGHA1 expression in T cells) should reflect contamination rather than intrinsic gene expression. Moreover, Applicants hypothesized that the levels of such off-target gene expression could serve as an accurate indicator of contamination rates in the entire dataset. To test this hypothesis, Applicants compared the mean expression levels of genes within each group (i.e. “within-group” expression) to their mean expression levels in all other cells (i.e. “non-group” expression), which Applicants used as a proxy for the composition of extracellular RNA (e.g. B cells vs. non-B cells, FIG. 39, see “Normalization and scaling of expression levels for contamination filtering” below for details). As expected, known markers for cell groups were enriched at the edges of the point distribution, where the difference between “within-group” and “non-group” expression was greatest. For example, known B cell markers were enriched on the left edge of the point distribution (e.g. IGHA1 and IGJ, FIG. 39), while markers for other cell types were enriched on the right edge, likely reflecting droplet contamination (e.g. CD3D and TPSAB1, FIG. 39). Furthermore, Applicants noticed two other patterns that yielded insights into droplet contamination: first, genes with sufficiently high “non-group” expression always had positive “within-group” expression, and second, there was a strong linear relationship between “within-group” and “non-group” expression levels, particularly for the potential contaminants on the right edge of the point distribution (FIG. 39). Taken together, these observations suggest that contamination uniformly affects all genes and that overall levels of contamination for each gene are proportional to its representation in the extracellular RNA pool.

Therefore, to estimate the contamination rate for each cell group, Applicants fit a robust linear model to the genes on the right edge of the point distribution, whose expression is likely driven by contamination. Surprisingly, the fitted models were nearly identical across groups (slope=1.33±0.07, intercept=−7.22±0.33) and Applicants constructed a consensus model using the mean slope and mean intercept. This model corresponds to a contamination rate between 0.5% and 5% of the total RNA pool in each sample. Applicants used this model to identify potential contaminants in all cell subsets by conservatively flagging genes with residuals <5 (i.e. 32-fold increase over the estimated contamination rate) and genes in each cell subset whose expression did not exceed 1% of its total expression across all cells. This approach filtered out nearly all known contamination throughout the full dataset.

Normalization and scaling of expression levels for contamination filtering. To estimate the contamination rate, Applicants compared the within-group and non-group expression levels of each gene (see above, FIG. 39).

To estimate the droplet contamination rate, Applicants compared for each gene its within-group and non-group expression levels (e.g. B cells vs. non-B cells, FIG. 39). However, because the composition of extracellular RNA varies across samples, contamination can have different effects within each sample. For example, cells derived from EPI samples have high levels of contaminating MUC2, while cells from LP samples have high levels of contaminating IGHA1. To account for these differences across samples, Applicants used a weighted mean to compute the non-group expression levels for each gene, where the weights were chosen to match the sample distribution of the target cell group.

Gene specificity. For each expressed gene, Applicants tested whether that gene was specific to any cell subset (e.g. T_(regs)) or any node of the cell hierarchy (e.g. CD4⁺ T cells). Applicants defined a gene as specific to a cell group, if it was significantly and positively DE in all pairwise comparisons to non-overlapping cell subsets and its mean expression level within the group was at least 2-fold higher than its mean expression in all other cell subsets. Additionally, Applicants searched for cases where a gene gained, lost, or changed its cell specificity between health and disease. As such cases may reflect differences in statistical power between the two cohorts, rather than changes in gene specificity, Applicants required that another cell subset have significantly higher expression of the gene in the appropriate group of cells (i.e. healthy subjects or UC patients, depending on the hypothesis being tested).

Using receptor-ligand pairs to infer cell-cell interactions. To identify cell-cell interactions, Applicants used the FANTOM5 database of literature supported receptor-ligand interactions. These receptors and ligands were mapped onto the lists of cell subset markers and DE genes within healthy, UC non-inflamed, and UC inflamed cells. To focus on genes that were enriched within a cell subset, Applicants considered a gene to be expressed within a cell only if its adjusted p-value was less than 0.05 and its discrete coefficient was greater than 1. In addition, to examine changes in cell-cell interactions with disease state, Applicants mapped the DE genes onto this network, removing edges that were not affected by DE, or adding edges in which both genes were DE.

For DE genes, receptors and ligands require that at least one gene within the interaction is differentially expressed. Because many genes showed relatively small changes in gene expression, Applicants required that all DE genes also be found as cell subset markers in either the healthy cells or cells isolated from the corresponding health state. In this way, Applicants constructed a network of cell-cell interactions, where each node is a cell type, each edge is a receptor-ligand interaction that is expressed.

Various modifications and variations of the described methods, pharmaceutical compositions, and kits of the invention will be apparent to those skilled in the art without departing from the scope and spirit of the invention. Although the invention has been described in connection with specific embodiments, it will be understood that it is capable of further modifications and that the invention as claimed should not be unduly limited to such specific embodiments. Indeed, various modifications of the described modes for carrying out the invention that are obvious to those skilled in the art are intended to be within the scope of the invention. This application is intended to cover any variations, uses, or adaptations of the invention following, in general, the principles of the invention and including such departures from the present disclosure come within known customary practice within the art to which the invention pertains and may be applied to the essential features herein before set forth. 

1. A method of detecting inflammatory bowel disease (IBD) comprising measuring in a biological sample obtained from the gastrointestinal tract of a subject the frequency of one or more cell types selected from the group consisting of B cells, T cells, endothelial cells, epithelial cells, fibroblasts and myeloid cells compared to the total of all cell types in the sample, wherein IBD is detected when the frequency of one or more cell types is altered as compared to a healthy frequency, preferably, wherein the one or more cell types are selected from the group consisting of colitis-associated inflammatory fibroblasts (CAIFs), absorptive transit amplifying (TA) 1 cells, absorptive TA 2 cells, class switching B cells, crypt fibroblasts (loFos), glial cells, goblet 1 cells, neutrophils, plasma B cells, post-capillary venules and tolerogenic DCs; and/or wherein the cell type is detected by measuring one or markers for each cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12; and/or wherein IBD comprises Crohn's disease or ulcerative colitis (UC); and/or wherein the biological sample is obtained by colonoscopy.
 2. (canceled)
 3. (canceled)
 4. The method of claim 1 further comprising measuring in the biological sample obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of: a) MTRNR2L1, HLA-B, CHI3L1, EIF5A, RPL3, S100P, TIMP1, REG1A, C8orf4, HMGCS2, DMBT1, AC005540.3, OLFM4, IL13RA2, MMP3, REG4, IGJ, DEFA5, TNFRSF12A, BGN, SELENBP1, TPM4, IFITM2, TNFRSF11B, PKM, PHLDA1, MT1G, LGALS4, IGFBP5, URAD, ANXA2, HLA-DRA, PLA2G2A, PDPN, S100A11, SELL, SOD2, LDHA, SMDT1, CCL8, FCGRT, RPL9, CYR61, NNMT, LMNA, HIF1A, CD82, LINC00152, TAGLN2, IFITM3, EMP1, AKR1C1, CD63, FKBPlA, PTMA, COL6A3, REG3A, BACE2, C10orf99, CNN3, CEBPB, RPL13A, LCN2, HSPA1B, CKB, PHGR1, CD59, Cllorf96, ANXA5, RPL18A, COL4A1, CTHRC1, PCOLCE, COL1A1, FTL, EMP3, GEM, COL4A2, PRSS23, S100A6, S100A3, CA1, REG1B, TNC, CCR7, MEOX1, FGF7, MMP1, RPS3A, THY1, RPS26, PKIB, CHP2, SERPINE1, TXNIP, COL6A1, RPS4Y1, PSME2, CAV1, ANGPTL2, TAGLN, TFF1, HGF, PDIA3, CDH13, ACADS, KDELR2, NOP10, SELM, HAPLN3, FABP4, PTGES, DSTN, CCL5, VAMP8, MT-ND1, SERPINHI, HYI, POLR2L, PPIB, HLA-DMA, TST, AQP1, SPARC, CA2, CCL13, MT-CYB, HLA-DPB1, SPINK1, AQP8, ATOX1, RPL37A, IER3, ENOl, MT1H, HSPA5, HSPA1A, ITM2C, SDC2, ID1, AMN, FABP6, PIGZ, COL8A1, DUOXA2, TPM2, CRIP2, HYAL2, CPXM1, NCOA7, RPS29, TMEM258, CLDN7, PHLDA2, TMSB10, F2R, PXMP2, SRM, CFB, NDUFA4L2, CBX3, NXPE4, ACAA2, NDRG2, KANSL1-AS1, KLF2, LAPTM4A, ITGA5, DHRS4, CDX2, PRKCDBP, RPL6, SOCS3, GPR160, PPDPF, SEPP1, TMEM141, ELP5, NRG1, SPON2, CXCL1, ID3, PTRF, CALR, TMEM165, HSP90B1, CLEC9A, INHBA, SPHK1, FABP1, LGALS2, PDLIM4, TMEM158, CKMT1A, TRMT112, CCDCl₃, HOXB13, MRGPRF, CALU, ACSF2, MMP10, VSIG2, RAMP1, MT1M, APOA4, TFPI2, FXYD3, MORF4L1, PEBP1, STAP2, NFKBIA, MT-C03, DHRS11, SPINT2, PRRX2, RCN3, EIF4A1, TUBB, TSHZ2, KRT8, ACTN1, VAMP5, RPL10, IL11, AGT, SERPINA1, SLC26A2, CLU, APOBEC3B, DNAJB1, THBS2, UBD, PIM3, PRKAR1A, IL32, IGFBP7, UGT2A3, HLA-DRB5, PPA1, CHCHD10, COL6A2, CD55, RNASET2, CTGF, MT-CO1, CTSK, C19orf10, SERPINE2, HSD17B12 and SAA1; or b) MTRNR2L1, HLA-B, RPL3, TIMP1, IGJ, IFITM2, CCR7, CCL5 and IGFBP7, preferably, wherein MTRNR2L1, HLA-B, TIMP1, CCR7, IFITM2, and IGFBP7 are upregulated as compared to a healthy reference level and wherein RPL3, IGJ and CCL5 are downregulated as compared to a healthy reference level; or c) genes in Table 4, 6, 8, 13, 14 or 15, wherein the genes or polypeptides are differentially expressed in IBD as compared to a healthy gastrointestinal tract reference level.
 5. (canceled)
 6. The method of claim 1, comprising measuring in B cells obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of: a) G0S2, FABP1, TNFRSF18, PHGR1, AGR2, GAS6, RPL3, LMNA, TIMP1, SMOC1, HIST1H1C, HSP90AA1, TNFRSF4, HSPA1A, HSPA1B, CYP20A1, KRT19, CXCR4, DNAJB1, XBP1, GOLGA2 and CADM1; or b) TIMP1, RPL3, HSP90AA1, LMNA, ILVBL, CD69, CTHRC1, TNFRSF4, GOS2, PABPC4, ITM2C, AGR2, RPS3A, RNASE6, LGALS4, HLA-DMA, FXYD3, PTMA, TNFRSF18, RP11-16E12.2, H3F3B, KLF6, QPRT, TPM4 and SMOC1; or c) C12orf75, METAP2, CCND3, HLA-DQB1, HLA-DRB5, RPS4Y1, TUBB2A, LCK, RMI2, SMARCB1, HLA-DPB1, TCEA1, MME, RPL9, SLBP, CD63, UBE2D3, A4GALT, PLD4, SIT1, PPP1CC, PAIP2, CCDC109B, DCAF12, SRSF3, HLA-DQA1, HLA-C, ISG20, HMGN1, HMCES, HNRNPC, HLA-DPA1, TUBB2B, HNRNPA3, CD27, EIF1AY, ITGAE, TPD52, ECHS1, RAP1B, HLA-DQA2, GGA2, CHCHD10, ACTR3, HLA-DRA, SGPP1, PGAM1, DCK, TSG101, HNRNPM, LTB, CLIC4, LSM10, GDI2, RGS16, CAPG, SRSF2, ZFAND2A, RPL36, CBX3, AGR2, MRPL47, TRA2A, FBL, SELT, SUMO2, HADHB, DEF8, FGD2, LIMD2, PSIP1, RBBP7, BZW1, TSTD1, MTF2, IKZF1, RUVBL1, BACH2, PIM1, CHRAC1, EZR, MCM5, IGJ, COX6B1, PRPSAP2, TK1 and CCR7.
 7. The method of claim 1, comprising measuring in endothelial cells obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of: a) PLAT, AQP1, CD9, HLA-A, HLA-DRA, EGLN3, LDHB, HLA-C, RBP5, CD99, PASK, S100A10, SERPINE1, CXCL12, JUN, ANXA2, TESC, IGJ, FOSB, LIMS1, HSPA1A, CALU, RCN3, S100A6, CST3, PRSS23, SEPP1, HSPA1B, WWTR1, RAMP1, GPX4, PSMB9, PSME2, CTGF, CD82, LGALS4, SNED1, TNFRSF4, IER3, VAMP8, ALDOA, HLA-B, TAP1, CD36, F2RL3, KDR, COL15A1 and PLAU; or b) PTGS1, RAMP1, PDLIM1, HLA-A, OLFML3, PLAT, STXBP6, UBD, LY6E, TNFSF10, CD9, MGP, CPE, PSMB8, PHLDA1, EIF4A2, GIMAP7, TMEM100, CST3, HLA-C, RPL9, RPL10, LPCAT4, AQP1, GIMAP1, SRPX, MALAT1, RPL3, AGR2, PRSS23, COL4A3BP, EFEMP1, SNHG7, TUBAIB, PTGES, NFKBIZ, B2M, FTH1, C19orf66, CDKN3, RNF181, EEF1B2, MDK, CLIC1, TPTEP1, TFF3, S100A10, JUN, CRIP1 and MED24; or c) PLAT, CXCL12, ENPP2, TXNIP, IGFBP4, CD36, ANXA2, OAZ2, CD320, AQP1, CTGF, RGS5, TGFBR2, RAMP1, CD9, C16orf80, CXCR4, CLDN5, STC1, GJA1, FAM213A, PLAU, HLA-E, PRKCDBP, RBP5, RPL9, SAT1, TNFSF10, S100A4, TSPAN7, AKR1C3, C8orf4, HLA-DPB1, SRP14, TNFRSF4, TIMP1, ANXA1, Clorf54, RND1, ANGPT2, EGR1, STAT3, SH3BP5, RPL29, CTNNBIP1, LSMD1, HLA-C, RBM17, GYPC, NDUFA7, IER2, COTL1, RPLPO, SDPR, IDI1, SLC6A6, RPL10A, MYL6, AQP3, NKX2-3, COASY and SOD2; or d) FAM222B, RP11-490M8.1, TWF2, ZNF205 and HYI.
 8. The method of claim 1, comprising measuring in epithelial cells obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of: a) SPINK1, PLA2G2A, IL18, ATP1B3, MTRNR2L1, GSTP1, GPX2, CYBA, TAX1BP3, S100A14, NQO1, TSPAN3, NAALADL1, CTSA, RARRES3, OAS1, LGALS1, HMGCS2, PCK1, PRDX5, MUC1, TMEM37, KRTCAP3, MT2A, MX1 and S100A11; or b) PTGS1, ESYT2, SHC1, HPGDS, HOOK1, BCKDK and RALGAPA1; or c) SPINK4, NUPR1, S100A14, BAIAP2L1, BDKRB1, MT-ND2, FAM3B, MUC13, TFF1, ANO9 and TUBB2A; or d) REG1A, CD74, RPL3, HLA-DRB1, MT2A, RPS3A, ARHGDIB, TIMP1, LIN7C, MTRNR2L1, KCNK6, RPL18A, TNFRSF12A and SEC11C; or e) HLA-DRA, HLA-DRB1, RARRES2, ID3, HLA-DMA, UGT2B17, CD74, HLA-DRB5, REG1A, HLA-DPB1, HLA-DPA1 and GLB1L2; or f) AGR2, HLA-DRA, CD74, S100A11, HSPB1, SPINK1, HLA-DRB1, TIMP1, RARRES3, SELENBP1, GPX2, MUC12, ID3, ARHGDIB, REG1A, PLA2G2A, CEACAM5, IDH2, IGJ, RNASET2, BSG, PSMB9, ADIRF, LEFTY1, RARRES1, LYZ, MTRNR2L1, TFF1, RPS4Y1, SRSF6, CNPY2, GSTP1 and ATP1B3; or g) RARRES2, ARHGDIB, IGJ, BST2, PKIG, PITX1, ETS2, HLA-DRA, TIMP1, MTRNR2L1, HRCT1, ZNF90, MUC12, AKR1B1, HLA-DPA1, VAMP7, S100P, NQO1, DEK, ABRACL, REG1A, ACAT1, DNAJB1, HLA-DRB1 and IGFBP4; or h) SPINK4, ITLN1, IGJ, AGR2, SDF2L1, TIMP1, PDLIM1, MUC2, LYZ, SELK, HMGCS2, SEC11C, SSR4, DNAJA1, FKBP11, REG4, EZR, SELM, CISD1, SYTL1, PHLDA2 and CHIPF.
 9. The method of claim 1, comprising measuring in fibroblasts obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of: a) COL1A2, GBP1, IFI27, DYNLT1, PKM, PHLDA1, DUSP1, CNOT4, CCL8, LAP3, ACP5, GSTT1, GALNT11, PSMB9, TNIP2, PSMB8, HAPLN3 and PERP; or b) NET1; or c) PDLIM7, NBL1, C12orf75, PHLDA2, IGFBP5, PRSS23, TM4SF1, SQRDL, MRGPRF, RERG, MXRA8, RPS4Y1, EGR1, HOXD9, TDO2, DUSP1, LMNA, CYB5R3, DDAH2 and TFPI2; or d) MMP2, SRPX2, TNC, MMP1, S100A4, NSG1, EDNRB, AGT, TRPA1, CPE, VSTM2A, RBP4, TSHZ2, IL32, VASN, CRIP1, NR4A2, PCTP, PRSS23, MCL1, NDUFA4L2, ANXA1, TMSB4X, PDLIM1, IGFBP3, CEBPD, FOXF1, ACP1, CiS, FRZB, ECM1, DMKN, ID4, PDGFRA, GADD45B and SPARCL1; or e) TM4SF1, VASN, GSN, FGF7, PLAT, CLEC14A, IQGAP2, ID3, FN1, SEPP1, TNXB, CCL13, TPBG, HSD17B2, STMN2, GPX3, VIM and TNFSF10; or f) GPX3, NR4A1, CIS, TM4SF1, DUSP1, ID1, LGALS3BP, COL15A1, SERPINGI, TNFAIP6, CFD, ADAMDEC1, MZT2B, MIF, EGR1, DKK3, NBEAL1, GSN, GGT5, FOXF1, RPL9 and CD74.
 10. The method of claim 1, comprising measuring in macrophages obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of LGMN, RNASE1, AKR1B1, LGALS2, A2M, C15orf48, VMO1, SERPINFI, SPINT1, ACP5, TFF3, RNASET2, ENPP2, LGALS1, MMP9, CORO1A, CSTB, SELK, MT2A, FBP1, PLSCR1, FXYD5, NR1H3, UCHL3, SEPP1 and AGR2.
 11. The method of claim 1, comprising measuring in T cells obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of: a) NUB1, CAV1, EIF2S1, COL6A1, POSTN, ALAS1 and RGCC; or b) S100A4, RPS29, TIMP1, RPL9, CFL1, VIM, ANXA1, PHLDA1, S100A11 and HLA-A; or c) IGJ and ADSS; or d) CCL3, CCL4, RPL10, RPL6, CD3E, MTRNR2L1, ARHGDIB, CD3G, RPL3, ITGB2, KLRB1, IFNG, RPL22, RPL18A and PTMA; or e) RPL9, EMP3 and ARFRP1; or f) CD7, CD2, TIAl and GRSF1; or g) RPL9, PFN1, IL32, ANXA1, S100A4, ARPClB, KLRB1, RPL30, ANAPC5, GAPDH, B2M, RPS28, PSME2, AK5, SERF2, RILPL2, RPS29, TAGLN2, FXYD5, S100A11, ANXA5, S100A6, PNRC1, ARPC2 and ZFP36; or h) ENTPD1, CD2, EIF5A, LCK, HAVCR2, ATP5L, KLRB1, CALR, MTPN, CENPA and MIF.
 12. The method of claim 1, comprising measuring in cells obtained from the gastrointestinal tract of the subject the expression of a gene or polypeptide selected from the group consisting of: a) AQP1, RPL3, RPS4Y1, LYZ, LCN2, 1D3, HLA-DRA, HLA-DRB1, HLA-DMA, HLA-DPA1, C2, NQO1, B2M, ARHGDIB, DNAJB1, RARRES2, MTRNR2L1, HLA-C, CD74, C19orf70, GSTT1, TESC, IFI27, PSME1, HMGCS2, HLA-DRB5, RPL6, UGT2B17, HLA-DPB1, PSMB9 and SCARB2; or b) RARRES2, HLA-DRA, SEC11C, MT2A, NIPSNAP1, OLFM4, DDC, MDK and CD82; or c) ALDH1A1, CLU, ANXA1, SPP1, IL32, CAPS, FIBIN, RPL3, RPL9, HLA-G, MRPS6, LINC00152, HOXC6, CDKN2A, TUBA1A, HLA-DQA2, SOCS3, SEPP1, IGJ, HLA-DRB5, KLC1, HLA-DRB1, NDUFB4, ENTPD2, SRGN, PMEPA1, HSPA1B, FKBPlA, GLIPR2, UBR4, UBB, COX7A1, LSM3, PRDX2 and NUPR1; or d) CST3, MARCKSL1, CD52, PPA1, IGJ, SERPINB1, TYMP, STMN1, FCER1A, DNAJB1 and PRELID1; or e) NFKBIZ, EGR3, IL1RL1, HLA-B, CAPG, EGR2, HLA-C, RPS4Y1, CTSW, EIF4G2 and ZEB2; or f) TFF3, ATP2A3, GSDMD, EMP3, IL12RB1, PSMD11, ENPP2, ALOX5AP and AKl; or g) TXN; or h) GBP1, FCGR2B, GSTO1, RPL30, TMEM176B, EMG1 and GDI2; or i) ILF3, CALCOCO2 and CD47.
 13. The method according to claim 1, wherein the cell type is obtained by sorting cells based on expression of one or markers for each cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12, preferably, wherein sorting is performed by deconvolution of bulk expression data in silico.
 14. (canceled)
 15. (canceled)
 16. A method of treating IBD comprising modulating the activity of one or more gastrointestinal tract cell types selected from the group consisting plasma B cells, class switching B cells, follicular B cells, microvascular cells, post-capillary venules, vitamin metabolizing, endothelial pericytes, enterocytes, tuft cells, goblet 2, absorptive TA 1, secretory TA, absorptive TA 2, cycling TA, goblet 1, stem cells, enteroendocrine, glial cells, inflammatory fibroblasts, fibroblast pericytes, myofibroblasts, villus fibroblasts, crypt fibroblasts (hiFos), crypt fibroblasts (loFos), T cells, macrophages, dendritic cells, mast cells, cycling monocytes, tolerogenic DCs, neutrophils, activated CD4 cells loFos, activated CD4 cells hiFos, CD8 IELs, CD8 LP cells, Tregs, memory T cells, NK cells and cycling CD8 cells, preferably, wherein the one or more cell types express one or more IBD GWAS genes selected from the group consisting of: a) IL32, MHCII, RNF186 and SLC39A8: or b) LMAN2, ATF4, TRIB1, HSPA6, RABEP2, CAMP, TSPAN14, STRN4, MOB2, HYAL1, DOCK9, CTSA, TST, PLEKHG6, RHPN2, C2CD2L, D2HGDH, REG4, DDC, HCK, MED16, GRB7, SPRED2, COG5, ADK, RIT1, SLC15A3, PLAU, ING5, NF2, PDLIM7, ZP1, PLA2G4A, CCL13, TTYH3, NFKBIZ, VPS11, CARD9, TNNI2, RIPK2, GPBAR1, SLC11A1, IFNG, CD28, EIF3G, CUL1, FASLG, MXD3, TCF19, DPAGT1, PHTF1, HOXA5, COX15 and LIF: or c) CCR10, GPRC5D, GPR18, CXCR5, CALCRL, F2RL3, FZD4, SlPRl, GPR4, APLNR, FZD6, LPAR6, GPR146, AVPR2, HRH1, GPRC5B, TBXA2R, GPRC5A, FZD5, GPR39, LGR5, VIPR1, F2RL1, LGR4, OPN3, FFAR4, GPR153, GPR37L1, FZD3, LPAR1, GPR137, SMOX, ADORA2B, BDKRB1, PGF, ADRA2A, PTGIR, EDNRA, MRGPRF, F2R, EDNRB, GLP2R, PTGFR, ACKR3, FZD1, ADORA1, ADORA3, CMKLR1, FPR3, P2RY13, ADRB2, LPAR5, P2RY14, GPR34, PTAFR, CCRL2, GPBAR1, FFAR2, C5AR1, C3AR1, CCR1, FPR1, GPR82, CXCR6, CCR7, DHX15, CCR6, GPR68, PTGDR and LTB4R: or d) TNFRSF17, SEMA4A, EBI3, RAMP3, ROBO4, F2RL3, APLN, NRP2, CCL21, ICAM2, PLXND1, HRH1, EPHA2, CGN, CELA3B, CFTR, RGMB, SCT, AZGP1, TSPAN1, IL22RA1, IL1R2, RSPO3, NRXN1, NCAM1, ANGPTL2, TNC, MMP1, COL18A1, C1QTNF1, COL5A3, NEO1, NTN1, BMP2, TSLP, SEMA3A, PROS1, ANGPTL1, CCL19, CD4, LY96, IL5RA, SIRPA, IL23A, IL1B, OSM, OLR1, KLRC2, CXCR6, IL17RA, KLRC1, ADAM10 and TNF; or e) CTSA, TNIP1, SEPHS2, AGPAT2, MIDN, FAM132A, SLC26A3, CHP2, SULT1A2, TMEM171, SULTIA1, Clorfl06, HNF4A, PLEKHG6, FUT2, CEBPA, GSDMB, EDN3, PTK6, PSORSICI, RHPN2, VDR, SLC26A6, AGPAT3, MST1R, NGEF, EFNA2, C2CD2L, ITPKA, SLC22A5, SLC35D1, AGXT, NXPE4, SLC39A8, TMEM258, F12, D2HGDH, BCL2L15, CFTR, GOT1, PLK1, ERGICI, ITLN1, REG4, SULT2B1, CCDCl60, CACNA2D2, SLC19A3, AGFG2, PLXNB1, DDC, C2orf54, LFNG, SNAPC4, MEX3A, GCG, GPBAR1, RXFP4, UCKL1, HCK, CAMP, BLM, SOX4, IFT172, RNF186, SMURF1, RNF123, TREH, HOXA11-AS, NOS2, C2CD4D, CEBPG, IL10RB, PRKCD, MED16, SEC16A, PPP1R12C, FOXO1, EPS8L1, TRIM31, CDH1, APOBR, SCNN1A, GRB7, SLC22A23, FRYL, ACHE, SMAD3, MAGI3, SPRED2, SMPD3, FAM83E, IL1R2, USP12, PWP2, ABCA7, SYT7 and COG5.
 17. (canceled)
 18. An isolated gastrointestinal tract cell characterized by expression of one or markers for a cell type selected from Table 1 A-D, Table 9, Table 11 or Table
 12. 19. A method for isolating, detecting or quantifying gastrointestinal tract cells in a biological sample of a subject, the method comprising: detecting or quantifying in the biological sample gastrointestinal tract cells as defined in claim 18, preferably, wherein the gastrointestinal tract cell is detected or quantified using one or more markers for a cell type selected from Table 1 A-D, Table 9, Table 11 or Table 12: or isolating from the biological sample gastrointestinal tract cells as defined in claim 18, preferably, wherein the gastrointestinal tract cell is isolated using one or more surface markers for a cell type selected from Table 1 A-D, Table 9, Table 11 or Table
 12. 20. (canceled)
 21. (canceled)
 22. (canceled)
 23. The method according to claim 19, wherein the gastrointestinal tract cells are isolated, detected or quantified using a technique selected from the group consisting of RT-PCR, RNA-seq, single cell RNA-seq, western blot, ELISA, flow cytometry, mass cytometry, fluorescence activated cell sorting, fluorescence microscopy, affinity separation, magnetic cell separation, microfluidic separation, and combinations thereof.
 24. The method of claim 16, wherein the method is for modulating the gastrointestinal tract cell composition comprising treating a subject with an agent capable of targeting intestinal stem cells to differentiate, preferably, wherein the intestinal stem cells are targeted to differentiate into absorptive transit amplifying (TA) 1 cells, absorptive TA 2 cells or class switching B cells.
 25. (canceled)
 26. (canceled)
 27. The method of claim 16, wherein the method is for modulating the gastrointestinal tract cell composition or activity comprising treating a subject with an agent capable of targeting a receptor-ligand interaction in the gut, preferably, wherein the receptor-ligand interaction comprises: a) CCR7 and one or more of CCL19 and CCL21: b) TNFB and LTBR; c) LGR5 and RSPO3; d) IL15 and IL15RA, e) FGF23 and FGFR1; f) CCL8 and CCR1; g) CXCL2 and XCR1; or h) XCL2 and XCR1.
 28. (canceled)
 29. The method of claim 1, wherein the method is for detecting drug resistance in inflammatory bowel disease (IBD) comprising measuring in a biological sample obtained from the gastrointestinal tract of the subject the frequency of colitis-associated inflammatory fibroblasts (CAIFs) compared to the total of all cell types in the sample, wherein drug resistance is detected when the frequency of CAIFs is altered as compared to a healthy frequency, preferably, wherein the drug resistance is resistance to anti-TNF therapy.
 30. (canceled)
 31. The method according to claim 29, wherein the cell type is detected by measuring one or markers selected from the group consisting of MMP3, MMP10, PLAU, IL1R1, IL13RA2, CXCL6, CCL11, TNFSF11 and TNFRSF11B. 